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USRE48025E1 - Obstructive sleep apnea treatment devices, systems and methods - Google Patents

Obstructive sleep apnea treatment devices, systems and methodsDownload PDF

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USRE48025E1
USRE48025E1US14/693,836US201514693836AUSRE48025EUS RE48025 E1USRE48025 E1US RE48025E1US 201514693836 AUS201514693836 AUS 201514693836AUS RE48025 EUSRE48025 EUS RE48025E
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nerve
stimulation
electrode
cuff
signal
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Stephen L. Bolea
Thomas B. Hoegh
Bruce J. Persson
Robert E. Atkinson
Sidney F. Hauschild
Paula M. Kaplan
Brian D. Kuhnley
Keith E. Jasperson
Wondimeneh Tesfayesus
Christopher K. Thorp
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Livanova USA Inc
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Abstract

In one embodiment, a method for maintaining patency of an upper airway of a patient to treat obstructive sleep apnea may include delivering an electrical stimulation to a portion of a superior laryngeal nerve via a nerve cuff when the nerve cuff is adjacent an external surface of the superior laryngeal nerve, the nerve cuff having a plurality of electrodes, wherein the nerve cuff is configured to be connected to an electrical stimulator via a stimulation lead.

Description

CROSS-REFERENCE TO RELATED APPLICATIONS
This patent application is a reissue application of U.S. Pat. No. 8,428,727 B2, which issued on Apr. 23, 2013, from U.S. patent application Ser. No. 13/093,534, filed on Apr. 25, 2011, which is a continuation of application Ser. U.S. patent application Ser. No. 11/907,533, filed on Oct. 12, 2007, of Stephen L. Bolea et al., entitled OBSTRUCTIVE SLEEP APNEA TREATMENT DEVICES, SYSTEMS AND METHODS, currently pending, now U.S. Pat. No. 8,417,343 B2, issued on Apr. 9, 2013, which claims the benefits of priority under 35 U.S.C. §§119 and 120 to U.S. Provisional Patent Application Nos. 60/851,386 and 60/918,257, filed on Oct. 13, 2006, and Mar. 14, 2007, respectively, the disclosures of all of which are expressly incorporated by reference herein. The entire contents of these applications are incorporated herein by reference. This reissue application is related to reissue application Ser. No. 14/681,764, filed on Apr. 8, 2015.
FIELD OF THE INVENTION
The inventions described herein relate to devices, systems and associated methods for treating sleeping disorders. More particularly, the inventions described herein relate to devices, systems and methods for treating obstructive sleep apnea.
BACKGROUND OF THE INVENTION
Obstructive sleep apnea (OSA) is highly prevalent, affecting one in five adults in the United States. One in fifteen adults has moderate to severe OSA requiring treatment. Untreated OSA results in reduced quality of life measures and increased risk of disease including hypertension, stroke, heart disease, etc.
Continuous positive airway pressure (CPAP) is a standard treatment for OSA. While CPAP is non-invasive and highly effective, it is not well tolerated by patients. Patient compliance for CPAP is often reported to be between 40% and 60%.
Surgical treatment options for OSA are available too. However, they tend to be highly invasive (result in structural changes), irreversible, and have poor and/or inconsistent efficacy. Even the more effective surgical procedures are undesirable because they usually require multiple invasive and irreversible operations, they may alter a patient's appearance (e.g., maxillo-mandibulary advancement), and/or they may be socially stigmatic (e.g., tracheostomy).
U.S. Pat. No. 4,830,008 to Meer proposes hypoglossal nerve stimulation as an alternative treatment for OSA. An example of an implanted hypoglossal nerve stimulator for OSA treatment is the Inspire™ technology developed by Medtronic, Inc. (Fridely, Minn.). The Inspire device is not FDA approved and is not for commercial sale. The Inspire device includes an implanted neurostimulator, an implanted nerve cuff electrode connected to the neurostimulator by a lead, and an implanted intra-thoracic pressure sensor for respiratory feedback and stimulus trigger. The Inspire device was shown to be efficacious (approximately 75% response rate as defined by a 50% or more reduction in RDI and a post RDI of ≤20) in an eight patient human clinical study, the results of which were published by Schwartz et al. and Eisele et al. However, both authors reported that only three of eight patients remained free from device malfunction, thus demonstrating the need for improvements.
SUMMARY OF THE INVENTION
To address this and other unmet needs, the present invention provides, in exemplary non-limiting embodiments, devices, systems and methods for nerve stimulation for OSA therapy as described in the following detailed description.
BRIEF DESCRIPTION OF THE DRAWINGS
It is to be understood that both the foregoing summary and the following detailed description are exemplary. Together with the following detailed description, the drawings illustrate exemplary embodiments and serve to explain certain principles. In the drawings:
FIG. 1 is a schematic diagram showing a fully implanted neurostimulator system with associated physician programmer and patient controller for treating obstructive sleep apnea;
FIG. 2 is a schematic diagram showing the implantable components ofFIG. 1 implanted in a patient;
FIG. 3 is a perspective view of the implantable components shown inFIG. 1;
FIG. 4 is a detailed perspective view of the implantable neurostimulator (INS) shown inFIG. 3;
FIG. 5 is a detailed perspective view of the nerve cuff electrode and lead body shown inFIG. 3;
FIG. 5a is an illustration of exemplary movements a lead body may be configured to withstand;
FIG. 6 is a close-up detailed perspective view of the nerve cuff electrode shown inFIG. 3;
FIG. 7 is a detailed perspective view of the internal components of the nerve cuff electrode shown inFIG. 6;
FIG. 8 shows side and end views of an electrode contact of the nerve cuff electrode shown inFIG. 7;
FIGS. 9A and 9B are perspective views of the respiration sensing lead shown inFIG. 3;
FIG. 10 schematically illustrates surgical access and tunneling sites for implanting the system illustrated inFIG. 2;
FIGS. 11A and 11B schematically illustrate dissection to a hypoglossal nerve;
FIGS. 12 and 12A-12D schematically illustrate various possible nerve stimulation sites for activating muscles controlling the upper airway;
FIGS. 13-22 and 22A-22D are schematic illustrations of various stimulation lead body and electrode designs for use in a neurostimulator system;
FIGS. 23-24 schematically illustrate alternative implant procedures and associated tools for the stimulation lead;
FIG. 25 schematically illustrates an alternative bifurcated lead body design;
FIGS. 26A-26B schematically illustrate alternative fixation techniques for the stimulation lead and electrode cuff;
FIG. 26C schematically illustrates an alternative embodiment of a stimulation lead having a fixation mechanism;
FIGS. 27A-27H schematically illustrate field steering embodiments;
FIGS. 27I-27Q schematically illustrate alternative embodiments of nerve cuff electrodes with selective fiber stimulation mechanisms;
FIGS. 28-33B schematically illustrate alternative fixation techniques for the respiration sensing lead;
FIG. 34 schematically illustrates the distal portion of an exemplary respiration sensing lead
FIGS. 35A-35E and 36 schematically illustrate alternative electrode arrangements on the respiration sensing lead;
FIGS. 37 and 37A-37C schematically illustrate various anatomical positions or bio-Z vectors for the electrodes on the respiration sensing lead;
FIG. 38A illustrates an exemplary method of sampling a plurality of vector signals;
FIGS. 38B-46 schematically illustrate alternative respiration signal processing techniques;
FIG. 47 schematically illustrates an alternative respiration detection technique;
FIGS. 47A-47D illustrate an exemplary stimulation trigger algorithm;
FIGS. 48-50 schematically illustrate alternative stimulation trigger algorithms;
FIG. 50A illustrates an exemplary waveform of a patient's respiratory cycle;
FIG. 50B illustrates an exemplary stimulation waveform;
FIGS. 51A-51M are schematic illustrations of various external (partially implanted) neurostimulation systems for treating obstructive sleep apnea;
FIGS. 52A-52G are schematic illustrations of a specific embodiment of an external (partially implanted) neurostimulation system;
FIGS. 53-56 schematically illustrate alternative screening tools; and
FIGS. 57A-58B schematically illustrate alternative intra-operative tools.
DETAILED DESCRIPTION OF EXEMPLARY EMBODIMENTS
The following detailed description should be read with reference to the drawings in which similar elements in different drawings are numbered the same. The drawings, which are not necessarily to scale, depict illustrative embodiments and are not intended to limit the scope of the invention.
Description of Fully Implanted Neurostimulator System
With reference toFIG. 1, aneurostimulator system10 including implantedcomponents20,physician programmer30 and patient controller40 is shown schematically. The implanted components of thesystem10 may generally include an implanted neurostimulator (INS)50 (a.k.a., implanted pulse generator (IPG)), an implanted stimulation lead (or leads)60, and an implanted respiration sensing lead (or leads)70. TheINS50 generally includes aheader52 for connection of theleads60/70, and a hermetically sealedhousing54 for the associated electronics and long-life or rechargeable battery (not visible). Thestimulation lead60 generally includes alead body62 with a proximal connector and a distalnerve electrode cuff64. Therespiration sensing lead70 generally includes alead body72 with a proximal connector and one ormore sensors74 disposed on or along a distal portion thereof. Suitable designs of theINS50,stimulation lead60 andrespiration sensing lead70 are described in more detail hereinafter.
As shown inFIG. 2, and by way of example, not limitation, the implanted components20 (shown faded) of theneurostimulator system10 are implanted in a patient P with theINS50 disposed in a subcutaneous pocket, thestimulation lead body62 disposed in a subcutaneous tunnel, thenerve cuff electrode64 disposed on a nerve (e.g., hypoglossal nerve (HGN)) innervating a muscle (e.g., genioglossus muscle, not shown) controlling the upper airway, the respirationsensing lead body72 disposed in a subcutaneous tunnel, and therespiration sensors74 disposed adjacent lung tissue and/or intercostal muscles outside the pleural space.
Generally, electrical stimulus is delivered by theINS50 via thestimulation lead60 to a nerve innervating a muscle controlling upper airway patency to mitigate obstruction thereof. To reduce nerve and muscle fatigue, the stimulus may be delivered for only a portion of the respiratory cycle, such as during inspiration which corresponds to negative pressure in the upper airway. Stimulation may be thus triggered as a function of respiration as detected byrespiration sensing lead70 in a closed-loop feedback system. By way of example, the stimulus may be triggered to turn on at the end of expiration (or at the beginning of inspiration), and triggered to turn off at the beginning of expiration (or at the end of inspiration). Triggering the stimulus as a function of expiration improves capture of the entire inspiratory phase, including a brief pre-inspiratory phase of about 300 milliseconds, thus more closely mimicking normal activation of upper airway dilator muscles. Over-stimulation may cause nerve and/or muscle fatigue, but a 40% to 50% duty cycle may be safely tolerated, thus enabling limited over-stimulation. As an alternative, stimulus may be delivered independent of actual respiration wherein the stimulus duty cycle is set for an average inspiratory duration at a frequency approximately equal to an average respiratory cycle.
Stimulus may be delivered to one or more of a variety of nerve sites to activate one muscle or muscle groups controlling patency of the upper airway. For example, stimulation of the genioglossus muscle via the hypoglossal nerve moves or otherwise stiffens the anterior portion of the upper airway, thereby decreasing the critical pressure at which the upper airway collapses during inspiration and reducing the likelihood of an apnea or hypopnea event occurring during sleep. Because the systems described herein work at the level of the tongue, it may be desirable to combine this therapy with a therapy (e.g., UPPP or palatal implant) that work at the level of the soft palate, thus increasing efficacy for a broader range of patients.
With reference back toFIG. 1, thephysician programmer30 may comprise acomputer32 configured to control and program theINS50 via a wireless link to aprogramming wand34. Thephysician programmer30 may be resident in a sleep lab where the patient undergoes a polysomnographic (PSG) study during which the patient sleeps while theINS50 is programmed to optimize therapy.
The patient controller40 may comprise control circuitry and associated user interface to allow the patient to control the system via a wireless telemetry link while at home, for example. The patient controller40 may include apower switch42 to turn the system on and slowly ramp up when the patient goes to sleep at night, and turn it off when the patient wakes in the morning. Asnooze switch44 may be used to temporarily put theINS50 in standby mode during which electrical stimulus is paused for a preprogrammed period of time to allow the patient to temporarily wake, after which theINS50 turns back on and ramps up to the desired stimulus level. Adisplay46 may be provided to indicate the status of the INS50 (e.g., on, off or standby), to indicate satisfactory wireless telemetry link to theINS50, to indicate remaining battery life of theINS50, to indicate normal operation of theINS50, and/or to indicate the need for patient action etc.Display46 may be configured to be a dash-board-like display, and may be any suitable display available to those of ordinary skill in the art, such as, for example, an LED or LCD display. Furthermore, information may be communicated to the patient controller40 for display purposes by any suitable means known to those of ordinary skill in the art. For example, communication of information may be achieved through inductively coupled or radio frequency telemetry. The patient controller40 may also have programmability to adjust stimulus parameters (e.g., amplitude) within a pre-set range determined by the physician in order to improve efficacy and/or to reduce sensory perception, for example. Optionally, the patient controller40 may be configured to function as theprogramming wand34 of thephysician programmer30.
Furthermore, the patient controller40 may be provided with one or more mechanisms for improving patient compliance. For example, patient controller40 may be provided with a time-keeping mechanism having the capabilities of a conventional alarm clock. In certain embodiments, controller40 may be programmed by the user and/or the physician to alert the user when action, such as, for example, turning thesystem10 on or off, is required by the user. Controller40 may be configured to alert the user by any suitable means known in the art. For example, controller40 may emit an audible alarm at programmed time intervals. In other embodiments, the patient controller40 may be used to monitor a patient. For example, the patient controller40 may be programmed to periodically send reports of patient actions, patient compliance, system status, etc., to a clinician or caregiver via a telephone or computer network.
With reference toFIG. 3, the implantedcomponents20 are shown schematically with more detail. The implanted components includeINS50,stimulation lead60, andrespiration sensing lead70. TheINS50 includesheader52 andhousing54. Thestimulation lead60 includeslead body62 andnerve cuff electrode64. Therespiration sensing lead70 includeslead body72 and respiration sensors74 (e.g., impedance sensing electrodes).
With reference toFIG. 4, theINS50 is shown schematically in more detail. TheINS50 includesheader52 that may be formed using conventional molding or casting techniques and may comprise conventional materials such as epoxy or polyurethane (e.g., Tecothane brand polyurethane). Thehousing54 may be formed using conventional stamping or forming techniques and may comprise conventional materials such as titanium or ceramic. Thehousing54 may include one or more isolated electrodes, and/or if a conductive material is used for thehousing54, thehousing54 may comprise an electrode, which may be used for respiratory sensing, for example. Thehousing54 may be hermetically sealed to theheader52 using conventional techniques. Theheader52 may include two or more receptacles for receiving the proximal connectors66/76 of thestimulation lead body62 and respirationsensing lead body72. The connectors66/76 may comprise a conventional design such as IS1 or other in-line designs. Theheader52 may also include set screw seals and blocks56 for receiving set screws (not shown) that establish electrical contact between theINS50 and the conductors of theleads60/70 via connectors66/76, and that establish mechanical fixation thereto. Some electrical contact may be achieved through spring type or cam-locked mechanisms. As shown, two setscrew arrangements56 are shown for thestimulation lead60 and four setscrew arrangements56 are shown for therespiration sensing lead70, but the number may be adjusted for the number of conductors in each lead. A hole58 may be provided in theheader52 for securing theINS50 to subcutaneous tissue using a suture at the time of implantation.
TheINS50 may comprise a conventional implanted neurostimulator design used in neurostimulation applications, such as those available from Texcel (US), CCC (Uruguay) and NeuroTECH (Belgium), but modified for the present clinical application in terms of stimulation signal parameters, respiratory signal processing, trigger algorithm, patient control, physician programming, etc. The INS may contain a microprocessor and memory for storing and processing data and algorithms. Algorithms may be in the form of software and/or firmware, for example. One of several different embodiments of the neurostimulator may be implemented. For example, the neurostimulator may be an internal/implanted neurostimulator (INS) powered by a long-life primary battery or rechargeable battery, or an external neurostimulator (ENS) wirelessly linked (e.g., inductive) to an implanted receiver unit connected to the leads. The INS (or the receiver unit of the ENS) may be implanted and optionally anchored in a number of different locations including a subcutaneous pocket in the pectoral region, the dorsal neck region, or cranial region behind the ear, for example.
TheINS50 may include any suitable circuitry and programming in accordance with the principles of the present disclosure. In one embodiment,INS50 may include an activity sensor (not shown) for sensing the activity of a patient, including the amount of activity of the patient. The activity sensor may detect motion of a patient by any suitable means available to those of ordinary skill in the art. For example, a patient's motion may be detected by, for example, using an internal accelerometer and/or measuring the impedance of the patient's torso with, for example, the built-in respiration sensor discussed below, and/or measuring a tissue pressure on the surface of the implantedINS50.
The data corresponding to a patient's detected motion may be stored, evaluated, and utilized in any of a number of various ways. In one embodiment, data corresponding to a patient's motion may be used to determine whether a patient is sleeping or awake. For example, when a patient's activity level falls below a predetermined threshold, it may be assumed that the patient is sleeping. Conversely, when the patient's activity level rises above the pre-determined threshold, it may be assumed that the patient is awake. The activity sensor therefore may be used to facilitate selectively applying treatment when the patient is detected to be sleeping and/or inhibiting treatment when the patient is detected to be awake. Alternatively, data corresponding to a patient's motion may be evaluated over a long period of time, such as, for example, the first few months of treatment, for indications of improvement in a patient's quality of life. It is contemplated that increases in a patient's average level of daily activity will correspond to successful treatment of OSA. This, in turn, may correspond to improvements in the patient's quality of life.
Moreover, theINS50 may include a long-life battery (not shown) which requires periodic replacement after years of service. Alternatively, the INS may include a rechargeable power source such as a rechargeable battery or super capacitor that is used instead of the long-life battery. To facilitate recharging, the INS may include a receiver coil inductively linked to a transmitter coil that is connected to a recharging unit powered by a larger battery or line power. Because the patient is stationary while sleeping, recharging may be scheduled to occur sometime during sleep to eliminate the need to carry the recharging unit during daily activities. The transmitter coil and the receiver coil may be arranged coaxially in parallel planes to maximize energy transfer efficiency, and may be held in proximity to each other by a patch, garment, or other means as described with reference to the external neurostimulator embodiments. Other examples of neurostimulator designs will be described in more detail hereinafter.
With reference toFIG. 5, thestimulation lead60 may comprise a variety of different design embodiments and may be positioned at different anatomical sites. For example, a nerve cuff electrode(s)64 may be attached to a nerve(s) innervating musculature affecting patency of the upper airway. As an alternative or in addition, thenerve cuff electrode64 may be replaced with an intramuscular electrode and placed directly in the musculature affecting patency of the upper airway. Thenerve electrode64 may be attached to a specific branch of a nerve innervating the desired muscle(s), or may be attached to a proximal trunk of the nerve in which a specific fascicle innervating the desired muscle(s) is targeted by steering the stimulus with multiple electrodes. One or more electrodes may be used for attachment to one or more portions of nerves on one side (unilateral) of the body, or one or more electrodes may be used for attachment to one or more portions of nerves on both sides (bilateral) of the body. Variations inlead body62 andelectrode64 design as well as variations in the target stimulation site or sites will be described in more detail hereinafter.
With continued reference toFIG. 5, thelead body62 may be sigmoid shaped, for example, to reduce strain applied to thecuff electrode64 when thelead body62 is subject to movement. The sigmoid shape, which may alternatively comprise a variety of other waveform shapes, may have a wavelength of approximately 1.0 to 1.5 cm, and an amplitude of approximately 0.75 to 1.5 cm, for example. Thelead body62 may comprise a tubular jacket withelectrical conductors68 extending therein. The tubular jacket may comprise extruded silicone having an outside diameter of approximately 0.047 inches and an inside diameter of approximately 0.023 inches, for example. The tubular jacket may optionally have a covering of co-extruded polyurethane, for example, to improve durability. Theconductors68, shown in a transparent window in the jacket for purposes of illustration only, may comprise a bifilar coil of insulated (e.g., ETFE) braided stranded wire (BSW) of MP35NLT material. The number ofconductors68 is shown as two, but may be adjusted depending on the desired number of independent electrodes used.
The various embodiments of stimulation leads, for example,stimulation lead60, disclosed herein may be fabricated by any suitable means known to those having ordinary skill in the art, and may be made from any suitable material. For example, the discussed sigmoid shape of the tubular jacket oflead body62 may be formed by first extruding silicone in a semi-cured or semi cross-linked state. Next, the semi cross-linked extruded tubular jacket may be placed in a sigmoid mold and then allowed to become fully cross-linked. In particular, the semi cross-linked extruded tubular jacket may be placed in an oven and heated to convert the semi cross-linked silicone of the extruded tubular jacket to fully cross-linked silicone. Additionally, a lumen within the tubular jacket may be created along a longitudinal axis of the tubular jacket by any suitable means.
Furthermore, in accordance with the principles of the present disclosure, it is contemplated that one or more of the various embodiments of stimulation leads disclosed herein may be implanted in or near highly mobile portions of the body. For example, embodiments of the disclosed stimulation leads may be implanted in the ventral neck, for example, along a path between the clavicle and mandible of a patient. Additionally, although mastication, deglutition, and speech may result in mechanical loading on an implanted stimulation lead, it has been found that gross movement of the head and neck may create high mechanical stresses in the conductors of the lead body, lead jacket, and the junction between the conductor wires and the anchor points, such as, for example, the electrodes. Accordingly, it may be desirable to configure the various embodiments of stimulation leads to withstand certain predetermined amounts of fatigue and/or stresses, which may result from mechanical loading on a lead body due to gross movements of a patient's neck and head.
In particular, research has revealed that approximately 98% of the population may experience a 38.5% elongation or less in the distance between the clavicle and angle of the mandible (e.g., adjacent a contemplated area of implantation for a stimulation lead in accordance with the principles of this disclosure). It has also been found that the angular range of motion of the cervical spine between adjacent vertebrae may be approximately 12 degrees, thereby flexing the lead through this angle with a bend radius assumed to be approximately 1.0 centimeter. See Augustus A. White III et al., Clinical Biomechanics of the Spine, pp. 84, 356, and 373 (1978). Furthermore, the frequency of gross head movement through the range of motion in the contemplated area of implantation has been estimated to be approximately 300,000 cycles per year, or on the average approximately 50 times per waking hour.
Thus, it may be desirable to design a lead body that is capable of withstanding, among other things, the stresses imparted by, the above-noted head and neck movements for an extended amount of time, such as, for example, ten years. In particular, in order to design a lead body that may remain functional for the exemplary ten year implanted life, it may be desirable to configure the lead bodies disclosed herein to withstand at least the above noted elongation and ranges of motion. For example, since implanted lead bodies are likely to be elongated by at least 38.5%, it may be desirable to design lead bodies to withstand being elongated by a predetermined distance Y, such as, for example, approximately 40% (+/−2%) from an initial unstressed state, for a minimum of 3.0 million cycles without failure, as depicted inFIG. 5A. In addition, since it is likely that an implanted lead body may experience an angular range of motion of at least 12 degrees, with a bend radius of approximately 1.0 centimeter, it may be desirable to configure the lead bodies to withstand being flexed around a predetermined radius X, such as, for example, 1.0 centimeter (+/−0.05 centimeters), for a predetermined amount of rotation W, such as, for example, from approximately 0 degrees to approximately 15 degrees (+/−3 degrees), such that the 15 degree maximum deflection occurs coincidentally with the maximum elongation of the lead body.
With reference toFIG. 6, thenerve cuff electrode64 may comprise acuff body80 having a lateral (or superficial)side82 and a medial (or contralateral, or deep)side84. Themedial side84 is narrower or shorter in length than thelateral side82 to facilitate insertion of themedial side84 around a nerve such that the medial side is on the deep side of the nerve and the lateral side is on the superficial side of the nerve. This configuration reduces the dissection of nerve branches and vascular supply required to get the cuff around a nerve. For the nerve cuff implant sites discussed herein, themedial side84 may have a length of less than 6 mm, and preferably in the range of approximately 3 to 5 mm, for example. Thelateral side82 may have a length of more than 6 mm, and preferably in the range of approximately 7 to 8 mm, for example. Thecuff body80 may be compliant and may be available in different sizes with an inside diameter of approximately 2.5 to 3.0 mm or 3.0 to 3.5 mm, for example. The cuff size may also be adjusted depending on the nominal diameter of the nerve at the site of implantation. Thecuff body80 may have a wall thickness of approximately 1.0 mm and may be formed of molded silicone, for example, and may be reinforced with imbedded fibers or fabrics. Anintegral tow strap86 may be used to facilitate wrapping the cuff around a nerve by first inserting thestrap86 under and around the deep side of the nerve and subsequently pulling the strap to bring themedial side84 in position on the deep side of the nerve and thelateral side82 on the superficial side of the nerve.
With continued reference toFIG. 6, thenerve cuff electrode64 includeselectrode contacts90A,90B, and90C imbedded in thebody80 of the cuff, with their inside surface facing exposed to establish electrical contact with a nerve disposed therein. A transverse guarded tri-polar electrode arrangement is shown by way of example, not limitation, wherein electrode contacts90A and90B comprise anodes transversely guardingelectrode contact90C which comprises a cathode.
With this arrangement, the anode electrodes90A and90B are connected to a common conductor68A imbedded in thebody80, and thecathode electrode90C is connected to an independent conductor68B extending from thelateral side82 to themedial side84 and imbedded in thebody80. By using theconductors68 to make connections within thebody80 of thecuff64, fatigue stresses are imposed on the conductors rather than theelectrode contacts90A,90B and90C.
With additional reference toFIGS. 7 and 8, theelectrode contacts90A,90B and90C may thus be semi-circular shaped having an arc length of less than 180 degrees, and preferably an arc length of approximately 120 degrees, for example. Eachelectrode90 may have two reverse bends (e.g., hooked or curled)portions92 to provide mechanical fixation to thebody80 when imbedded therein. Eachelectrode90 may also have twocrimp tabs94 defining grooves thereunder for crimping to theconductors68 or for providing a passthrough. As shown inFIG. 7, conductor68A passes through the grooves under thelower crimp tabs94 of electrodes90B and90A,loops98 around through the grooves under theupper crimp tabs94 of electrodes90A and90B, is crimped96 by theupper tabs94 of electrodes90A and90B to provide mechanical and electrical connection, is looped again back between thecrimp tabs94 on the outside of theelectrode contact90, and is resistance spot welded95 to provide redundancy in mechanical and electrical connection. Also as shown inFIG. 7, conductor68B passes through the groove under thelower crimp tab94 ofelectrode90C, loops around through the groove under theupper crimp tab94 ofelectrode90C, and is crimped by theupper tab94 ofelectrode90C to provide mechanical and electrical connection. This arrangement avoids off-axis tensile loading at the crimp sites96 which may otherwise fail due to stress concentration, and the loopedportion98 provides additional strain relief.
FIG. 8 provides example dimensions (inches) of anelectrode contact90 for a 2.5 mm inside diameter cuff, wherein the electrode is formed of 90/10 or 80/20 platinum iridium alloy formed by wire EDM, for example. As illustrated, and as exemplary and approximate dimensions,electrode contact90 may include a surface A having a full radius, a dimension B of 0.079 inches from tangent to tangent, a dimension C of 0.020 inches (3×), a radius of curvature D of 0.049R with a 16 micro-inch RMS, a dimension E of 0.008 inches (2×), a dimension F of 0.0065 inches (+/−0.001 inches) (2×), a dimension G of 0.006 inches (+0.002 inches, −0.001 inches) (2×), a dimension H of 0.014 inches (2×), a dimension I of 0.010 inches (2×), a dimension J of 0.010 inches (2×), and a dimension K of 0.006 inches (+/−0.001 inches).
With reference toFIGS. 9A and 9B, a distal portion of therespiration sensing lead70 and a distal detail of thesensing lead70, respectively, are shown schematically. In the illustrated embodiment, therespiration sensing lead70 and associatedsensors74 are implanted as shown inFIG. 2. However, the respiration sensor(s) may comprise a variety of different design embodiments, both implanted and external, and may be positioned at different anatomical sites. Generally, the respiratory sensor(s) may be internal/implanted or external, and may be connected to the neurostimulator via a wired or wireless link. The respiratory sensor(s) may detect respiration directly or a surrogate thereof. The respiratory sensor(s) may measure, for example, respiratory airflow, respiratory effort (e.g., diaphragmatic or thoracic movement), intra-pleural pressure, lung impedance, respiratory drive, upper airway EMG, changes in tissue impedance in and around the lung(s) including the lungs, diaphragm and/or liver, acoustic airflow or any of a number other parameters indicative of respiration. Detailed examples of suitable respiration sensing leads and sensors will be described in more detail hereinafter.
With continued reference toFIGS. 9A and 9B, therespiration sensing lead70 includes alead body72 and a plurality of respiration sensors74A-74D comprising ring electrodes for sensing bio-impedance. Thelead body72 of therespiration sensing lead70 may include a jacket cover comprising an extruded silicone tube optionally including a polyurethane cover (80A durometer), or may comprise an extruded polyurethane tube (55D durometer). The ring electrodes74A-74D may comprise 90/10 or 80/20 platinum iridium alloy tubes having an outside diameter of 0.050 inches and a length of 5 mm, and secured to the jacket cover by laser welding and/or adhesive bonding, for example. Thelead body72 may include a plurality ofconductors78 as seen in the transparent window in the jacket cover, which is shown for purposes of illustration only. Theconductors78 may comprise insulated and coiled BSW or solid wire (optionally DFT silver core wire) disposed in the tubular jacket, with one conductor provided for each ring electrode74A-74D requiring independent control. Generally, the impedance electrodes74A-74D may comprise current emitting electrodes and voltage sensing electrodes for detecting respiration by changes in bio-impedance. The number, spacing, anatomical location and function of the impedance electrodes will be described in more detail hereinafter.
System10 may also include a plurality of diagnostic mechanisms (e.g., circuitry and/or programming) for monitoring and/or determining the functionality of certain components, such as, for example,stimulation lead60. In particular,system10 may include one or more switching circuits (not shown) that facilitate connection of the respiratory/trans-thoracic impedance sensing circuits of the present disclosure (discussed in greater detail below) to stimulation lead60 for measuring the impedance oflead60. In some embodiments, the impedance sensing circuit may be connected to each electrode pair. In other embodiments, the impedance sensing circuit may be connected between the case of the implantedINS50 and eachconductor68 within thelead60. While those having ordinary skill in the art will readily recognize that any suitable impedance sensing method may be utilized to monitor and/or determine the functionality oflead60, the respiratory/trans-thoracic impedance sensing circuit of the present disclosure may be preferred, since this circuit may be capable of identifying small changes in impedance rather than the large changes detectable by standard methods.
As alluded to above, sensing the impedance oflead60 may provide for monitoring and/or determining the functionality oflead60. Specifically, sensing the impedance oflead60 may facilitate diagnosing and distinguishing between differing types of failures oflead60. In particular, research has revealed that changes in the impedance oflead60 may be indicative of certain types of failures, including, but not limited to, corrosion, high contact resistance, breakage, and/or shorting. For example, a broken wire inside the lead could be identified by an excessively high lead impedance value. Corrosion of an electrode with its resultant decrease in effective electrode surface area could be identified by a smaller increase in impedance of that electrode. Similarly, an abnormally low value could correspond with a short between conductors in the lead, or an abrasion of the lead body that exposed a conductor to the tissue. Measuring from the case of the INS to each electrode allows independent identification of the integrity of each wire/electrode in the lead. In addition, sensing the impedance oflead60 may facilitate periodic, automated adjustment of stimulation pulse amplitude so as to maintain constant current, energy, and/or charge delivery using a simpler voltage mode delivery circuit. Such automated adjustment may facilitate ensuring safety and effectiveness by consistently delivering the prescribed current, energy, or charge in the presence of tissue/electrode impedance variations. By consistently controlling the delivery of only the minimally required energy necessary for stimulation of the nerve, the stimulation amplitude may be programmed closer to the actual stimulation threshold rather than programming a wide margin to ensure continued effectiveness. This enhances safety and reduces power consumption. Moreover, sensing the impedance oflead60 may allow monitoring of certain system dynamics, such as, for example, doses actually delivered to a patient.
Description of Implant Procedure
With reference toFIG. 10, surgical access sites are schematically shown for implanting theinternal neurostimulator components20 shown inFIG. 1. Theinternal neurostimulator components20 may be surgically implanted in a patient on the right or left side. The right side may be preferred because it leaves the left side available for implantation of a pacemaker, defibrillator, etc., which are traditionally implanted on the left side. The right side may also be preferred because it lends itself to a clean respiratory signal less susceptible to cardiac artifact and also offers placement of respiratory sensors across the interface between the lung, diaphragm and liver for better detection of impedance changes during respiration.
With continued reference toFIG. 10, the INS (not shown) may be implanted in asubcutaneous pocket102 in the pectoral region, for example. The stimulation lead (not shown) may be implanted in asubcutaneous tunnel104 along (e.g., over or under) the platysma muscle in the neck region. The respiration sensing lead (not shown) may be implanted in a subcutaneous tunnel106 extending adjacent the ribcage to an area adjacent lung tissue and/or intercostal muscles outside the pleural space. The nerve cuff electrode (not shown) may be attached to a nerve by surgical dissection at asurgical access site110 proximate the targeted stimulation site. In the illustrated example, the target nerve is the right hypoglossal nerve and the surgical access site is in the submandibular region.
With reference toFIGS. 11A and 11B, asurgical dissection110 to the hypoglossal nerve is shown schematically. A unilateral dissection is shown, but a bilateral approach for bilateral stimulation may also be employed. Conventional surgical dissection techniques may be employed. The branch of the hypoglossal nerve (usually a medial or distal branch) leading to the genioglossus muscle may be identified by stimulating the hypoglossal nerve at different locations and observing the tongue for protrusion. Because elongation and/or flexion may be mistaken for protrusion, it may be desirable to observe the upper airway using a flexible fiber optic scope (e.g., nasopharyngoscope) inserted into the patient's nose, through the nasal passages, past the nasopharynx and velopharynx to view of the oropharynx and hypopharynx and visually confirm an increase in airway caliber by anterior displacement (protrusion) of the tongue base when the nerve branch is stimulated.
The implant procedure may be performed with the patient under general anesthesia in a hospital setting on an out-patient basis. Alternatively, local anesthesia (at the surgical access sites and along the subcutaneous tunnels) may be used together with a sedative in a surgical center or physician office setting. As a further alternative, a facial nerve block may be employed. After a post-surgical healing period of about several weeks, the patient may return for a polysomnographic (PSG) test or sleep study at a sleep center for programming the system and titrating the therapy. A trialing period may be employed prior to full implantation wherein the hypoglossal nerve or the genioglossus muscle is stimulated with fine wire electrodes in a sleep study and the efficacy of delivering stimulus to the hypoglossal nerve or directly to the genioglossus muscle is observed and measured by reduction in apnea hypopnea index, for example.
Other nerve target sites are described elsewhere herein and may be accessed by similar surgical access techniques. As an alternative to surgical dissection, less invasive approaches such as percutaneous or laparoscopic access techniques may be utilized, making use of associated tools such as tubular sheaths, trocars, etc.
Description of Alternative Stimulation Target Sites
With reference toFIG. 12, various possible nerve and/or direct muscle stimulation sites are shown for stimulating muscles controlling patency of the upper airway. In addition to the upper airway which generally includes the pharyngeal space, other nerves and dilator muscles of the nasal passage and nasopharyngeal space may be selectively targeted for stimulation. A general description of the muscles and nerves suitable for stimulation follows, of which the pharyngeal nerves and muscles are shown in detail inFIG. 12.
Airway dilator muscles and associated nerves suitable for activation include are described in the following text and associated drawings. The dilator naris muscle functions to widen the anterior nasal aperture (i.e., flares nostrils) and is innervated by the buccal branch of the facial nerve (cranial nerve VII). The tensor veli palatine muscle functions to stiffen the soft palate and is innervated by the medial (or internal) pterygoid branch of the mandibular nerve MN. The genioglossus muscle is an extrinsic pharyngeal muscle connecting the base of the tongue to the chin and functions to protrude the tongue. The genioglossus muscle is typically innervated by a distal or medial branch (or branches) of the right and left hypoglossal nerve. The geniohyoid muscle connects the hyoid bone to the chin and the sternohyoid muscle attaches the hyoid bone to the sternum. The geniohyoid muscle functions to pull the hyoid bone anterosuperiorly, the sternohyoid muscle functions to pull hyoid bone inferiorly, and collectively (i.e., co-activation) they function to pull the hyoid bone anteriorly. The geniohyoid muscle is innervated by the hypoglossal nerve, and the sternohyoid muscle is innervated by the ansa cervicalis nerve.
By way of example, a nerve electrode may be attached to a specific branch of the hypoglossal nerve innervating the genioglossus muscle (tongue protruder), or may be attached to a more proximal portion (e.g., trunk) of the hypoglossal nerve in which a specific fascicle innervating the genioglossus muscle is targeted by steering the stimulus using an electrode array. Activating the genioglossus muscle causes the tongue to protrude thus increasing the size of anterior aspect of the upper airway or otherwise resisting collapse during inspiration.
As an alternative to activation of any or a combination of the airway dilator muscles, co-activation of airway dilator and airway restrictor or retruder muscles may be used to stiffen the airway and maintain patency. By way of example, a nerve electrode may be attached to specific branches of the hypoglossal nerve innervating the genioglossus muscle (tongue protruder), in addition to the hyoglossus and styloglossus muscles (tongue retruders), or may be attached to a more proximal portion (e.g., trunk) of the hypoglossal nerve in which specific fascicles innervating the genioglossus, hyoglossus and styloglossus muscles are targeted by steering the stimulus using an electrode array. Activating the hyoglossus and styloglossus muscles causes the tongue to retract, and when co-activated with the genioglossus, causes the tongue to stiffen thus supporting the anterior aspect of the upper airway and resisting collapse during inspiration. Because the tongue retruder muscles may overbear the tongue protruder muscle under equal co-activation, unbalanced co-activation may be desired. Thus, a greater stimulus (e.g., longer stimulation period, larger stimulation amplitude, higher stimulation frequency, etc.) or an earlier initiated stimulus may be delivered to the portion(s) of the hypoglossal nerve innervating the genioglossus muscle than to the portion(s) of the hypoglossal nerve innervating the hyoglossus and styloglossus muscles.
With continued reference toFIG. 12, examples of suitable nerve stimulation sites include B; A+C; A+C+D; B+D; C+D; and E. Sites B and E may benefit from selective activation by field steering using an electrode array. As mentioned before, nerve electrodes may be placed at these target nerve(s) and/or intramuscular electrodes may be placed directly in the muscle(s) innervated by the target nerve(s).
Site A is a distal or medial branch of the hypoglossal nerve proximal of a branch innervating the genioglossus muscle and distal of a branch innervating the geniohyoid muscle. Site B is a more proximal portion of the hypoglossal nerve proximal of the branches innervating the genioglossus muscle and the geniohyoid muscle, and distal of the branches innervating the hyoglossus muscle and the styloglossus muscle. Site C is a medial branch of the hypoglossal nerve proximal of a branch innervating the geniohyoid muscle and distal of branches innervating the hyoglossus muscle and the styloglossus muscle. Site D is a branch of the ansa cervicalis nerve distal of the nerve root and innervating the sternohyoid. Site E is a very proximal portion (trunk) of the hypoglossal nerve proximal of the branches innervating the genioglossus, hyoglossus and styloglossus muscles.
Activating site B involves implanting an electrode on a hypoglossal nerve proximal of the branches innervating the genioglossus muscle and the geniohyoid muscle, and distal of the branches innervating the hyoglossus muscle and the styloglossus muscle.
Co-activating sites A+C involves implanting a first electrode on a hypoglossal nerve proximal of a branch innervating the genioglossus muscle and distal of a branch innervating the geniohyoid muscle, and implanting a second electrode on the hypoglossal nerve proximal of a branch innervating the geniohyoid muscle and distal of branches innervating the hyoglossus muscle and the styloglossus muscle.
Co-activating sites A+C+D involves implanting a first electrode on a hypoglossal nerve proximal of a branch innervating the genioglossus muscle and distal of a branch innervating the geniohyoid muscle; implanting a second electrode on the hypoglossal nerve proximal of a branch innervating the geniohyoid muscle and distal of branches innervating the hyoglossus muscle and the styloglossus muscle; and implanting a third electrode on a branch of an ansa cervicalis nerve distal of the nerve root and innervating the stemohyoid.
Co-activating sites B+D involves implanting a first electrode on a hypoglossal nerve proximal of branches innervating the genioglossus muscle and the geniohyoid muscle, and distal of branches innervating the hyoglossus muscle and the styloglossus muscle; and implanting a second electrode on a branch of an ansa cervicalis nerve distal of the nerve root and innervating the sternohyoid.
Co-activating sites C+D involves implanting a first electrode on a hypoglossal nerve proximal of a branch innervating the geniohyoid muscle, and distal of branches innervating the hyoglossus muscle and the styloglossus muscle and implanting a second electrode on a branch of an ansa cervicalis nerve distal of the nerve root and innervating the sternohyoid.
Activating site E involves implanting an electrode on a hypoglossal nerve proximal of the branches innervating the genioglossus, hyoglossus and styloglossus muscles; and selectively activating (e.g., by field steering) the genioglossus muscle before or more than the hyoglossus and styloglossus muscles.
With reference now toFIGS. 12A-12D, additional possible nerve stimulation sites are shown for effecting muscles controlling patency of the upper airway. For example, the cranial root of the accessory nerve AN (cranial nerve XI) innervates the levator veli palatini muscle of the soft palate, which elevates the soft palate. The cranial root of the accessory nerve AN also innervates the palatoglossal muscle, which functions to pull the soft palate inferiorly when the genioglossus is co-activated via the hypoglossal nerve (HGN). Moreover, because the cranial root of the accessory nerve AN also innervates various other muscles including, but not limited to, the palatopharyngeus, specific fibers in the accessory nerve AN may be selectively stimulated with one or more of the fiber selective stimulation means described in greater detail below, in order to only activate desired fibers of the nerve. The glossopharyngeal nerve GN (cranial nerve IX) innervates the stylopharyngeus, which functions to dilate the lateral walls of the pharynx. However, since the glossopharyngeal nerve GN is a multi-function nerve with both afferent and efferent fibers, one or more of the fiber selective stimulation means described in greater detail below may be used to facilitate targeting the fibers that innervate only the stylopharyngeus. The cranial root of the accessory nerve AN and the glossopharyngeal nerve GN may be singularly activated, or these nerves may be co-activated with other nerve sites, such as, for example, the hypoglossal nerve, for increased efficacy.
Another possible nerve stimulation site may include the superior laryngeal nerve SLN. The superior laryngeal nerve SLN descends posterior and medial from the internal carotid artery and divides into the internal laryngeal nerve ILN and external laryngeal nerve ELN. While the external laryngeal nerve ELN descends behind the sternohyoid with the superior thyroid artery, the internal laryngeal nerve ILN descends near the superior laryngeal artery. The internal laryngeal nerve ILN contains sensory (afferent) fibers that are connected to receptors in the larynx. Some of these receptors include, but are not limited to, mechanoreceptors which detect pressure changes in a patient's upper airway associated with its collapse and institute a physiological response to re-open the patient's upper airway. Therefore, stimulation of specific afferent fibers inside the ILN nerve may result in triggering a reflex response that causes upper airway dilation by activating several muscles groups.
As discussed below, the superior laryngeal nerve SLN, in addition to being a sensory nerve, is also a motor nerve. Therefore, it is contemplated that one or more of the fiber selective stimulation means described in greater detail below may be utilized to facilitate only stimulating the sensory or afferent fibers of the nerve.
Description of Alternative Nerve Electrodes
Any of the alternative nerve electrode designs described hereinafter may be employed in the systems described herein, with modifications to position, orientation, arrangement, integration, etc. made as dictated by the particular embodiment employed. Examples of other nerve electrode designs are described in U.S. Pat. No. 5,531,778, to Maschino et al., U.S. Pat. No. 4,979,511 to Terry, Jr., and U.S. Pat. No. 4,573,481 to Bullara, the entire disclosures of which are incorporated herein by reference.
With reference to the following figures, various alternative electrode designs for use in the systems described above are schematically illustrated. In each of the embodiments, by way of example, not limitation, the lead body and electrode cuff may comprise the same or similar materials formed in the same or similar manner as described previously. For example, the lead body may comprise a polymeric jacket formed of silicone, polyurethane, or a co-extrusion thereof. The jacket may contain insulated wire conductors made from BSW or solid wire comprising MP35N, MP35N with Ag core, stainless steel or Tantalum, among others. The lead body may be sigmoid shaped to accommodate neck and mandibular movement. Also, a guarded cathode tri-polar electrode arrangement (e.g., anode-cathode-anode) may be used, with the electrodes made of 90/10 or 80/20 PtIr alloy with silicone or polyurethane backing.
With specific reference toFIGS. 13A and 13B, a self-sizing and expandable design is shown to accommodate nerve swelling and/or over-tightening.FIG. 13A shows a perspective view of anerve electrode cuff130 on a nerve such as a hypoglossal nerve, andFIG. 13B shows a cross-sectional view of thenerve cuff electrode130 on the nerve. In this embodiment, the implantablenerve cuff electrode130 comprises acompliant sheet wrap132 configured to be wrapped about a nerve and secured thereto by connecting opposite portions of the sheet bysutures138, for example. Thesheet132 includes a plurality of radially and longitudinally distributedfenestrations134 to allow expansion of thesheet132 to accommodate nerve swelling and/or over tightening.Electrode contacts136 comprising a coil, foil strip, conductive elastomer or individual solid conductors may be carried by thesheet132 with an exposed inside surface to establish electrical contact with the nerve.
With specific reference toFIGS. 14A-14C, another self-sizing and expandable design is shown to accommodate nerve swelling and/or over-tightening.FIG. 14A shows a perspective view of anerve electrode cuff140 on a nerve such as a hypoglossal nerve, andFIG. 14B shows a cross-sectional view of thenerve cuff electrode140 on the nerve. In this embodiment, the implantablenerve cuff electrode140 comprises acompliant sheet wrap142 configured to be wrapped about a nerve and secured thereto by connecting opposite portions of the sheet by sutures148A, or by a buckle148B as shown inFIG. 14C, for example. The opposite portions of thesheet142 comprise one or morenarrow strips144 integral with thesheet142 to allow expansion and to accommodate nerve swelling and/or over tightening. Electrode contacts146 comprising a coil, foil strip, conductive elastomer or individual solid conductors may be carried by thesheet142 with an exposed inside surface to establish electrical contact with the nerve.
With specific reference toFIGS. 15A-15C, another self-sizing and expandable design is shown to accommodate nerve swelling and/or over-tightening.FIG. 15A shows a perspective view of anerve electrode cuff150 on a nerve such as a hypoglossal nerve, andFIG. 15B shows a cross-sectional view of thenerve cuff electrode150 on the nerve. In this embodiment, the implantablenerve cuff electrode150 comprises acompliant sheet wrap152 configured to be wrapped about a nerve and secured thereto by connecting opposite portions of thesheet152 bysutures158, for example. The opposite portions of thesheet152 are offset from the nerve and a thickened portion of thesheet152 fills the offset space. The offset distance reduces the amount of compressive force that the electrode cuff can exert on the nerve. To further reduce the pressure on the nerve, thesheet152 includes a plurality of radially distributedslits154 extending partly through the thickness of thesheet152 to allow expansion and to accommodate nerve swelling and/or over tightening.
With specific reference toFIGS. 16A and 16B, another self-sizing and expandable design is shown to accommodate nerve swelling and/or over-tightening.FIG. 16A shows a perspective view of anerve electrode cuff160 on a nerve such as a hypoglossal nerve, andFIG. 16B shows a cross-sectional view of thenerve cuff electrode160 on the nerve. In this embodiment, the implantablenerve cuff electrode160 comprises acompliant sheet wrap162 configured to be wrapped about a nerve and secured thereto by connecting opposite portions of thesheet162 bysutures168, for example. Thesheet162 includes a plurality of radially distributed and longitudinally extending convolutions164 that may comprise alternative thick164A and thin164B portions in thesheet162 and/or overlappingportions164C of thesheet162 to allow expansion and to accommodate nerve swelling and/or over tightening.Electrode contacts166 comprising a coil, foil strip, conductive elastomer or individual solid conductors may be carried by thesheet162 with an exposed inside surface to establish electrical contact with the nerve.Nerve cuff electrode160 may accommodate one or twolead bodies62A,62B for connection to theelectrode contacts166 on the same or opposite sides of the nerve.
Turning now toFIGS. 16C-16D, additional self-sizing and expandable designs are shown to accommodate nerve swelling and/or over-tightening. With specific reference toFIG. 16C, there is depicted a nerve cuff electrode1600 having a cuff body with a relatively wide semi-cylindricallateral side1601 and a plurality of opposingarms1602 extending thereform for placement on the deep (contralateral) side of the nerve. Although the embodiment depicted inFIG. 16C includes two such opposingarms1602, nerve cuff electrode1600 may include any suitable number of opposingarms1602.Lateral side1601 may include an array ofelectrode contacts1603. For example, in the depicted embodiment, lateral side may include threeelectrode contacts1603. The threeelectrode contacts1603 may include onecathode electrode contact1603 disposed between twoanode electrode contacts1603, as shown.
Arms1602 may be secured around a nerve (not shown) by any suitable means. For example, it is contemplated thatarms1602 may be elastic in nature, so as to gently grasp the nerve on its deep (contralateral) side. Alternatively,arms1602 may be actively secured about a nerve by, for example, suturing an end portion ofarms1602 to, e.g., a portion oflateral side1601. In embodiments wherearms1602 may be actively secured about a nerve,arms1602 may be provided with a safety mechanism (not shown) that permits nerve cuff electrode1600 to become disengaged from a nerve it is secured about upon the application of a predetermined amount of force. This predetermined force will be established at a level that is below that which can cause damage to the nerve.
As shown inFIG. 16D, opposingarms1602 may be configured to expand and/or deform as necessary, in order to accommodate nerve swelling caused by, for example, localized trauma inflicted upon the nerve during cuff implantation. For example, each of opposingarms1602 may have an unattachedterminal end1602a. In order to facilitate expansion, opposingarms1602 may be also made from any suitable material known to those having ordinary skill in the art. For example,arms1602 may be made from an elastomer, such as, for example, silicone or polyurethane. Additionally, one or both ofarms1602 may be provided with one or more limiting mechanisms (not shown) to limit the amount ofexpansion arms1602 may undergo as a result of, for example, nerve swelling. Such limiting mechanisms may include any suitable mechanism, including, but not limited to, flanges, barbs, and/or sutures.
With reference toFIG. 16E, there is depicted another design of a self-sizing and expandable nerve cuff electrode1610. For the purposes of this disclosure, nerve cuff electrode1610 may be substantially similar to nerve cuff electrode1600 depicted inFIGS. 16C-16D. Nerve cuff electrode1610, however, may differ from nerve cuff electrode1600 in at least two significant ways. First, for example,lateral side1611 of nerve cuff electrode1610 may carry twoanode electrode contacts1613 and themedial side1612 may carry onecathode electrode contact1613 in an arrangement that may be referred to as transverse guarded tri-polar. Second, for example, nerve cuff electrode1610 may include three arms1614-1616 extending fromlateral side1611. In the depicted embodiment,arms1614 and1616 may be configured to extend substantially in the same direction from thesame edge1611a oflateral side1611, whilearm1615 may be configured to extend in substantially the opposing direction from an opposing edge1611b oflateral side1611. In the depicted embodiment,arm1615 may be disposed betweenarms1614 and1616, and may be configured to carry thecathode electrode contact1613, as mentioned above. However, any suitable arrangement of arms1614-1616 and/orelectrode contacts1613 may be utilized within the principles of this disclosure.
As shown inFIG. 16F, certain embodiments of nerve curve electrode1600 and/or nerve cuff electrode1610 may include one or moreelongated arms1617.Arms1617 may include any suitable length, so as to allowarms1617 to wrap around a body portion of the cuff electrode one or more times in a spiral-like fashion, when the cuff electrode is mounted about an un-swollen nerve. However,arms1617 may allow the cuff electrode to remain mounted on the nerve as it accommodates large amounts of nerve swelling by unraveling and/or unwrapping as the nerve swells. For example, each of thearms1617 may overlaplateral side1601 or1611 to accommodate larger amounts of nerve swelling without allowing the cuff to become detached from the nerve. Theelongated arms1617 may extend around the body of the cuff electrode to form a spiral when the nerve is in a substantially unswollen state, as shown.
With reference toFIG. 17, a modularnerve electrode cuff170 is shown that includes asemi-cylindrical body portion172 with an array ofelectrode contacts176 with separateinsulative strips174 for placement on the deep (contralateral side) of the nerve, which typically has more nerve branches and connecting blood vessels. In this embodiment, independent placement of theelectrode body172 on the superficial (lateral) side of the nerve and placement of the insulative strips174 on the deep (contralateral) side of the nerve minimizes dissection. Thestrips174 may be connected to theelectrode body172 by sutures or buckles as described previously. This embodiment is also self-sizing to accommodate nerve swelling and/or over-tightening.
With reference toFIG. 18, anerve cuff electrode180 is shown that has a cuff body with a relatively wide semi-cylindricallateral side182 and a relatively narrow semi-cylindricalmedial side184 that may extend through a small fenestration around the deep (contralateral) side of a nerve to securely and gently grasp the nerve while minimizing dissection. In the illustrated example, thelateral side182 carries twoanode electrode contacts186 and themedial side184 carries onecathode electrode contact186 in an arrangement that may be referred to as transverse guarded tri-polar. Atow strap188 is provided for inserting themedial side184 around the deep side of the nerve. Thetow strap188 may be integrally formed with themedial side184 of the cuff body, and may include a reinforcedtip188A with a serrated or marked cut line188B.
With reference toFIGS. 19A and 19B, anerve cuff electrode190 is shown that has a cuff body with a relatively wide semi-cylindricallateral side192 and a relatively narrow semi-cylindricalmedial side194 that may extend through a small fenestration around the deep (contralateral) side of a nerve to securely and gently grasp the nerve while minimizing dissection. In the illustrated example, thelateral side192 carries onecathode electrode contact196C and two guarding anode electrode contacts196B and196D, and themedial side194 carries oneanode electrode contact196A in an arrangement that may be referred to as transverse and longitudinal guarded quad-polar. The provision of guardingelectrode contacts196B and196C reduces extrinsic stimulation due to the lack of insulative material on themedial side194. The embodiments ofFIGS. 18, 19A and 19B illustrate two different electrode contact arrangements, but the number and arrangement may be modified to suit the particular application.
With reference toFIG. 20, a nervecuff electrode array200 is shown that utilizes a series of relatively narrowindependent cuffs200A,200B and200C with corresponding independentlead bodies62. Providing a series of relatively narrowindependent cuffs200A,200B and200C minimizes the required dissection around the nerve for implantation thereof. Also, the series ofindependent cuffs200A,200B and200C allows more selectivity in electrode placement to adjust for anatomical variation or multiple target stimulation sites, for example. Providing multiple independentlead bodies62 allows for more options in routing and placement of the individual lead bodies62 (e.g., alternate placement oflead body62A) and also prevents tissue encapsulation around thelead bodies62 from collectively affecting encapsulation of the nerve cuffs200. Each of the cuffs200A,200B and200C may include acuff body202 with one or more imbedded electrode contacts (not shown) and atow strap204 as described before. Also, each of the cuffs200A,200B and200C may includesuture208 or abuckle206 to lock onto thetow strap204 for connecting opposite ends of thebody202 around the nerve.
With reference toFIGS. 21A and 21B, anerve cuff electrode210 is shown withmultiple electrode contacts216 radially spaced around the inside surface of a compliantsplit cuff body212 to establish multiple electrical contact points around the circumference of the nerve. Each of theelectrode contacts216 may be connected to independent conductors in thelead body62 via axially extendingwires217. This arrangement allows for field steering as discussed herein. The compliantsplit cuff body212 together with axially extendingwires217 allows for self-sizing to accommodate nerve swelling and/or over-tightening. One or more pairs oftabs214 extending from opposite end portions of thecuff body212 may be connected by a suture (not shown) as described herein. As shown inFIG. 21B, the proximal and distal ends of thecuff body212 may have taperedthickness extensions218 to provide strain relief and reduce mechanical irritation of the nerve due to contact with the edge of the cuff.
With reference toFIG. 22, anerve cuff electrode220 is shown with aseparable lead62 in what may be referred to as a modular design. In this embodiment, thenerve cuff electrode220 includes a semi-circular flexible cuff body (or housing)222 with areceptacle224 configured to accommodate a distal end of alead body62 therein. Thereceptacle224 may provide a releasable mechanical lock to thelead body52 as by a press fit, mating detents, etc. The distal end of thelead body62 carries an array ofring electrodes65, withwindows226 provided in thecuff body222 configured to align with thering electrodes65 and permit exposure of thering electrodes65 to the nerve to establish electrical connection therebetween. Thecuff body222 may be attached to the nerve or simply placed adjacent the nerve. Any of the cuff designs described herein may be provided with a receptacle to accommodate a removable lead body. This embodiment allows postoperative removal of thelead body62 without removal of thecuff220, which may be beneficial in revision operations, for example.
Turning now toFIG. 22A, there is depicted another design for anerve cuff electrode2000 where a substantially cylindricaldistal portion62′ oflead body62 carries an array ofelectrodes2001.Electrodes2001 may include ring electrodes that extend completely around the circumference oflead body62, or, alternatively, may include generally semi-circular electrodes that extend partially around the circumference oflead body62. The electrode may be selectively insulated on any portion of its surface to allow directional stimulation.Nerve cuff electrode2000 may further include a nerve securing mechanism for securinglead body62 to a nerve, such as, for example, a hypoglossal nerve. The nerve securing mechanism may include, for example, acompliant sheet wrap2002 that is attached on one end to a distal portion oflead body62, and unattached on the other opposing end.Compliant sheet wrap2002 may be attached to leadbody62 by any suitable means.
As shown inFIG. 22B,compliant sheet wrap2002 may be configured to be wrapped around a nerve and secured thereto by, for example, connecting opposite portions of thesheet wrap2002 together.Sheet wrap2002 may be provided with one or more features to facilitate such connections. For example, it is contemplated that a portion2002b ofsheet wrap2002 that is closest to leadbody62 may be provided with a projection2002c that is configured for insertion into acorresponding opening2002e provided on a portion2002d ofsheet wrap2002 that is opposite portion2002b.Opening2002e may be configured to retain projection2002c despite the forces exerted onsheet wrap2002 during normal nerve swelling. However,opening2002e may be configured to release projection2002c when forces greater than a predetermined threshold are exerted onsheet wrap2002, so as to prevent injury to the nerve. As shown inFIG. 22C, in some embodiments,opening2002e may be provided as a slot, which, in addition to securing projection2002c, may allow projection2002c to slide within theopening2002e, thereby allowing expansion of thesheet wrap2002 to accommodate nerve swelling and/or over tightening of thesheet wrap2002. Additionally, both portions2002b and2002d may be provided with suitable openings to facilitate the insertion of sutures (not shown) or other suitable fastening mechanisms.Sheet wrap2002 may have any desired width. For example,sheet wrap2002 may have a substantially tapered width, in order to securely wrap the nerve while minimizing dissection.
Compliant sheet wrap2002 may be provided with any of a number of means that allowsheet wrap2002 to expand, in order to accommodate nerve swelling and/or over tightening. For example, in one embodiment,sheet wrap2002 may be provided with a plurality of radially and/or longitudinally distributed fenestrations (not shown). In other embodiments,sheet wrap2002 may be provided with a plurality of undulations2002a, such as, for example, sigmoid undulations, which may allow for expansion ofsheet wrap2002.
With reference now toFIG. 22D, there is depicted another design for a nerve cuff electrode2200 where adistal portion62″ oflead body62 carries an array ofelectrodes2201. For the purposes of this disclosure, nerve cuff electrode2200 may include substantially the same features asnerve cuff electrode2000 depicted inFIGS. 22A-22C. Nerve cuff electrode2200, however, may differ fromnerve cuff electrode2000 in thatdistal portion62″ may be substantially flat or paddle-shaped. Furthermore,electrode contacts2201, rather than being circular or semi-circular in configuration, may be substantially flat in configuration. In certain procedures, it is contemplated that the paddle-shapeddistal portion62″, along with the substantiallyflat electrode contacts2201, may promote greater contact betweenelectrode contacts2201 and the nerve they are mounted upon.
Description of Alternative Implant Procedure for the Stimulation Lead
With reference toFIGS. 23A-23C, an insertable paddle-shapedlead230 design is shown. Theinsertable lead230 may have a paddle-shape (rectangular) cross-section with atubular jacket232 and one ormore conductors234 extending therethrough to one or more distally placed electrode contact(s)236. The electrode contact(s)236 may be imbedded in a molded distal end of thejacket232 such that theelectrode contact236 has an exposed surface to face the nerve when implanted as shown inFIG. 23B. The space between the nerve and electrode is shown for purposes of illustration only, as the electrodes may be placed in direct contact with the nerve.Soft tines238 may be integrally formed at the distal end of thetubular jacket232 for purposes of mild fixation to tissue when implanted. Theinsertable lead230 is configured to be placed adjacent to the nerve (thereby negating the need for a cuff) by inserting thelead230 at thesurgical access site110 and following the nerve distally until theelectrode contacts236 are placed adjacent the target stimulation site. Theinsertable lead232 may be used alone or in conjunction with another lead as shown inFIGS. 23B and 23C. In the illustrated example, afirst lead230A is inserted along a superficial side of the nerve and a second lead230B is inserted along a deep side of the nerve.
A method of implantinglead230 may generally comprise accessing a proximal extent of the nerve by minimal surgical dissection and retraction of the mylohyoid muscle as shown inFIG. 23C. Special tools may alternatively be employed for percutaneous or laparoscopic access as shown and described with reference toFIGS. 24A-24C. Subsequently, two paddle-shapedleads230 withdistal electrode contacts236 may be inserted into the surgical access site and advanced beyond the access site along a distal aspect of the nerve to the desired stimulation site on either side of the nerve. These techniques minimize trauma and facilitate rapid recovery.
A less invasive method of implanting a paddle-shapedlead230 is shown inFIGS. 24A-24C. In this embodiment, a rectangulartubular trocar240 with a sharpened curved tip is placed through apercutaneous access site111 until a distal end thereof is adjacent the superficial side of the nerve. A paddle-shapedlead230 is inserted through the lumen of thetrocar240 and advanced distally beyond the distal end of thetrocar240 along the nerve, until theelectrode contacts236 are positioned at the target stimulation site. As shown inFIG. 24B, which is a view taken along line A-A inFIG. 24A, theinsertable lead230 includesmultiple electrode contacts236 in an anode-cathode-anode arrangement, for example, on one side thereof to face the nerve when implanted. In this embodiment, tines are omitted to facilitate smooth passage of thelead230 through the trocar. To establish fixation around the nerve and to provide electrical insulation, abacker strap242 of insulative material may be placed around the deep side of the nerve. To facilitate percutaneous insertion of thebacker242, acurved tip needle244 may be inserted through a percutaneous access site until the tip is adjacent the nerve near the target stimulation site. Aguide wire246 with a J-shaped tip may then be inserted through theneedle244 and around the nerve. Thebacker242 may then be towed around using theguide wire246 as a leader, and secured in place by a buckle (not shown), for example.
With reference toFIG. 25, abifurcated lead250 is shown to facilitate separate attachment of electrode cuffs64 to different branches of the same nerve or different nerves for purposes described previously. Any of the nerve cuff electrode or intramuscular electrode designs described herein may be used with thebifurcated lead250 as shown. In the illustrated example, afirst lead furcation252 and a second lead furcation254 are shown merging into acommon lead body62. Eachfurcation252 and254 may be the same or similar construction as thelead body62, with modification in the number of conductors. More than twoelectrode cuffs64 may be utilized with corresponding number of lead furcations.
Description of Stimulation Lead Anchoring Alternatives
With reference toFIGS. 26A and 26B, anelastic tether264 with a limited length is utilized to prevent high levels of traction on theelectrode cuff64 around the hypoglossal nerve (or other nerve in the area) resulting from gross head movement. In other words,tether264 relieves stress applied to theelectrode cuff64 by thelead body62.FIGS. 26A and 26B are detailed views of the area around the dissection to the hypoglossal nerve, showing alternative embodiments of attachment of thetether264. The proximal end of thetether264 may be attached to thelead body62 as shown inFIG. 26A or attached to theelectrode cuff64 as shown inFIG. 26B. The distal end of thetether264 may be attached to the fibrous loop carrying the digastrics tendon as shown inFIG. 26A or attached to adjacent musculature as shown inFIG. 26B.
By way of example, not limitation, and as shown inFIG. 26A, a tubular collar262 is disposed on thelead body62 to provide connection of thetether264 to thelead body62 such that thelead body62 is effectively attached viasuture266 andtether264 to the fibrous loop surrounding the digastrics tendon. Thetether264 allows movement of the attachment point to the lead body62 (i.e., at collar262) until thetether264 is straight. At this point, any significant tensile load in the caudal direction will be borne on the fibrous loop and not on theelectrode cuff64 or nerve. This is especially advantageous during healing before a fibrous sheath has formed around thelead body62 andelectrode cuff64, thus ensuring that thecuff64 will not be pulled off of the nerve. It should be noted that the length of the tether262 may be less than the length of thelead body62 between the attachment point (i.e., at collar262) and thecuff64 when the tensile load builds significantly due to elongation of this section oflead body62.
Thetether264 may be formed from a sigmoid length of braided permanent suture coated with an elastomer (such as silicone or polyurethane) to maintain the sigmoid shape when in the unloaded state. Thetether264 may also be made from a monofilament suture thermoformed or molded into a sigmoid shape. The distal end of thetether264 may be attached to the fibrous loop using asuture266 or staple or other secure means. Note that thetether264 may be made from a biodegradable suture that will remain in place only during healing.
Also by way of example, not limitation, an alternative is shown inFIG. 26B wherein thetether264 is attached to theelectrode cuff64. The distal end of thetether264 may be attached to the adjacent musculature bysuture266 such the musculature innervated by branches of the hypoglossal nerve or other musculature in the area where theelectrode cuff64 is attached to the nerve. Thetether264 ensures that theelectrode cuff64 and the hypoglossal nerve are free to move relative to the adjacent musculature (e.g., hyoglossal). As significant tensile load is applied to thelead body62 due to gross head movement, thetether264 will straighten, transmitting load to the muscle rather then to the nerve orelectrode cuff64.
As alluded to above,stimulation lead60 may comprise a number of differing design embodiments. One such embodiment has been discussed above with respect toFIG. 5. Another such embodiment is depicted inFIG. 26C, which illustrates a stimulation lead2600. Stimulation lead2600 may be substantially similar to and/or may include one or more of the features described in connection withstimulation lead60. As shown inFIG. 26C, stimulation lead2600 may include a lead body2662 having a first, proximal lead body portion2663. First lead body portion2663 may be substantially similar to leadbody62. For example, first lead body portion2663 may include a similar flexibility aslead body62. Lead body2662 may further include a second, distallead body portion2664 leading to the distal end of lead body2662 at the nerve cuff electrode. Secondlead body portion2664 may include a material property that is different than lead body portion2663, such as, for example, a greater flexibility, in order to accommodate stresses imparted upon lead body2662 by a nerve cuff electrode and movement of the patient's head, neck, and other neighboring body portions. The highly flexibledistal portion2664 reduces the stress (torque and tension) imparted by lead body2662 on the electrode cuff, thereby reducing the likelihood that the cuff will be detached from the nerve or damage the nerve.
Leadbody portion2664 may be made more flexible than lead body portion2663 by any of a variety of ways. For example,lead body portion2664 may be made from a material having differing flexibility. Alternatively, the diameters of the braided stranded wires (BSW) and/or wire insulation that make up thelead body portion2664 may be reduced when possible.
With continuing reference toFIG. 26C, stimulation lead2600 may further include an anchor2665 operably connected to lead body2662. Although anchor2665 in the illustrated embodiment is depicted as being disposed in betweenlead body portions2663 and2664, anchor2665 may be disposed at any suitable location along the length of lead body2662. Furthermore, anchor2665 may be fixedly or movably connected to lead body2662.
Anchor2665 may include any suitable configuration known in the art. For example, anchor2665 may include a substantially flat body portion2666. Body portion2666 may be configured to be secured to tissue, such as, for example, tissue proximate a treatment site, by any suitable means available in the art. For example, body portion2666 may be provided withopenings2667 to facilitate, for example, suturing anchor2665 to nearby tissue. Anchor2665 can thereby isolate stress (tension) to one portion of lead body2662, and particularly portion2663, caused by gross head and neck movement.
Description of Field Steering Alternatives
With reference toFIGS. 27A-27G, a field steeringnerve cuff electrode64 is shown schematically. As seen inFIG. 27A, thenerve cuff electrode64 may include four electrode contacts90A-90D to enable field steering, and various arrangements of the electrode contacts90A-90D are shown inFIGS. 27B-27G. Each ofFIGS. 27B-27G includes a top view of thecuff64 to schematically illustrate the electrical field (activating function) and an end view of thecuff64 to schematically illustrate the area of the nerve effectively stimulated. With this approach, electrical field steering may be used to stimulate a select area or fascicle(s) within a nerve or nerve bundle to activate select muscle groups as described herein.
With specific reference toFIG. 27A, thenerve cuff electrode64 may comprise a cuff body having a lateral (or superficial)side82 and a medial (or contralateral, or deep)side84. Themedial side84 is narrower or shorter in length than thelateral side82 to facilitate insertion of themedial side84 around a nerve such that the medial side is on the deep side of the nerve and the lateral side is on the superficial side of the nerve. Anintegral tow strap86 may be used to facilitate wrapping the cuff around a nerve. Thenerve cuff electrode64 includeselectrode contacts90A,90B,90C and90D imbedded in the body of the cuff, with their inside surface facing exposed to establish electrical contact with a nerve disposed therein. Electrode contacts90A and90B are longitudinally and radially spaced from each other.Electrode contacts90C and90D are radially spaced from each other and positioned longitudinally between electrode contacts90A and90B. Each of the four electrode contacts may be operated independently via four separate conductors (four filar) in thelead body62.
With specific reference toFIGS. 27B-27G, each includes a top view (left side) to schematically illustrate the electrical field or activating function (labeled E), and an end view (right side) to schematically illustrate the area of the nerve effectively stimulated (labeled S) and the area of the nerve effectively not stimulated (labeled NS). Electrodes90A-90D are labeled A-D for sake of simplicity only. The polarity of the electrodes is also indicated, with each of the cathodes designated with a negative sign (−) and each of the anodes designated with a positive sign (+).
With reference toFIG. 27B, a tripolar transverse guarded cathode arrangement is shown with electrodes C and D comprising cathodes and electrodes A and B comprising anodes, thus stimulating the entire cross-section of the nerve.
With reference toFIG. 27C, a bipolar diagonal arrangement is shown with electrode C comprising a cathode and electrode A comprising an anode, wherein the fascicles that are stimulated may comprise superior fascicles of the hypoglossal nerve, and the fascicles that are not stimulated may comprise inferior fascicles of the hypoglossal nerve (e.g., fascicles that innervate the intrinsic muscles of the tongue).
With reference toFIG. 27D, another bipolar diagonal arrangement is shown with electrode D comprising a cathode and electrode B comprising an anode, wherein the fascicles that are stimulated may comprise inferior fascicles of the hypoglossal nerve.
With reference toFIG. 27E, a bipolar axial arrangement is shown with electrode A comprising a cathode and electrode B comprising an anode, wherein the fascicles that are stimulated may comprise lateral fascicles of the hypoglossal nerve.
With reference toFIG. 27F, a bipolar transverse arrangement is shown with electrode C comprising a cathode and electrode D comprising an anode, wherein the fascicles that are stimulated may comprise medial fascicles of the hypoglossal nerve.
With reference toFIG. 27G, a modified tripolar transverse guarded cathode arrangement is shown with electrode C comprising a cathode and electrodes A and B comprising anodes, thus stimulating the entire cross-section of the nerve with the exception of the inferior medial fascicles.
Nerves like the hypoglossal nerve or superior laryngeal nerve typically include a plurality of fibers having relatively larger diameters and a plurality of fibers having relatively smaller diameters. In the case of single function nerves, such as, for example, the hypoglossal nerve HGN, all of the nerve fibers may either be sensory or motor in function. However, in the case of multi-function nerves, such as, for example, the superior laryngeal nerve SLN, the fibers having relatively larger diameters are typically motor (efferent) fibers, and the fibers having relatively smaller diameters are typically sensory (afferent) fibers. Accordingly, there may be a need to selectively stimulate the differing diameter fibers in a nerve.
Turning now toFIG. 27H, there is depicted an embodiment of auni-directional stimulation electrode2700 having a distal end2700a and a proximal end2700b.Electrode2700 may include a substantiallycylindrical nerve cuff2701 in accordance with the principles of the present disclosure. As illustrated,nerve cuff2701 may include anouter surface2701a and an inner surface2701b.Electrode2700 may further include a plurality of electrode contacts2702-2704. Electrode contacts2702-2704 may be used as any suitable electrode contact known to those of ordinary skill in the art. For example,electrode contact2702 may be used as an anode, electrode contact2703 may be used as a cathode, andelectrode contact2704 may be used as a second anode. Electrode contacts2702-2704 may also include any suitable shape and/or configuration known in the art. For example, electrode contacts2702-2704 may include a substantially semi-circular configuration.
Electrode contacts2702-2704 may be disposed onnerve cuff2701 in any suitable configuration to achieve the desired effect. For example, electrode contacts2702-2704 may be disposed on inner surface2701b. As depicted inFIG. 27H, cathode electrode contact2703 may be disposed approximately equidistant from distal end2700a and proximal end2700b, andanode electrode contacts2702 may be differentially spaced around cathode electrode contact2703, so as to control the direction of stimulation ofelectrode2700. For example,anode electrode contact2702 may be spaced from cathode electrode contact2703 by any suitable distance χ while secondanode electrode contact2704 may be spaced from cathode electrode contact2703 by a distance that is approximately two or three times greater than distance χ. In this exemplary configuration, the direction of stimulation may be in the direction ofarrow2705.
In use,electrode2700 may be implanted upon a nerve in accordance with the principles of this disclosure.Electrode2700 may be oriented on the nerve it is implanted on in any suitable manner, such as, for example, according to the direction of intended stimulation. Thus, in circumstances where it may be desired to stimulate efferent (motor) fibers of a nerve, such as, for example, the superior laryngeal nerve SLN, while avoiding stimulation to afferent (sensory) fibers of the nerve, theelectrode2700 may be oriented on the nerve in a manner such thatanode electrode contact2702 is located distally of cathode electrode contact2703, with distal and proximal designations based on the relative location of the electrode contact on the nerve. Alternatively, in circumstances where it may be desired to stimulate afferent fibers of a nerve while avoiding stimulation of efferent fibers of the nerve, theelectrode2700 may be oriented on the nerve in a manner such thatanode electrode contact2702 is located proximally of cathode electrode contact2703.
With reference now toFIG. 27I, there is depicted an embodiment of a stimulation electrode2750 for, among other things, selectively stimulating differing diameter fibers of a nerve, such as, for example, the hypoglossal nerve or superior laryngeal nerve. Electrode2750 may include abody2751, and may include any suitable configuration in accordance with the principles of the present disclosure. Additionally, electrode2750 may include an array2752 of suitable electrode contacts known to those skilled in the art. Although the depicted embodiment of electrode2750 includes five electrode contacts2753a-2753e, array2752 may include a greater or lesser number of electrode contacts. Electrode contacts2753a-2753e may be disposed onbody2751 in any suitable configuration to produce the desired effect. For example, as depicted inFIG. 27I, electrode contacts2753a-2753e may be disposed serially, with approximately a one (1) millimeter spacing in between each electrode contact2753a-2753e. Electrode contacts2753a-2753e may be configured to function as either anode electrode contacts or cathode electrode contacts, as desired.
Electrode contacts2753 may be connected to an implanted neurostimulator (INS), such as, for example,INS50, in accordance with the present disclosure. The INS may be programmed to select any of electrode contacts2753a-2753e for nerve stimulation. For example, in circumstances where it may be desired to stimulate the smaller diameter fibers of a nerve, it is contemplated that all electrode contacts2753a-2753e may be selected for nerve stimulation, since closely spaced electrode contacts typically affect smaller diameter fibers (e.g., afferent or sensory fibers). In these circumstances, electrode contacts2753a,2753c, and2753e may function as anode electrode contacts and electrode contacts2753b and2753d may function as cathode electrode contacts. In circumstances where it may be desired to stimulate the larger diameter fibers of a nerve, it is contemplated that only electrode contacts2753a,2753c, and2753e may be selected for nerve stimulation, since loosely spaced electrode contacts typically affect larger diameter fibers (e.g., efferent or motor fibers). In these circumstances, electrode contacts2753a and2753e may function as anode electrode contacts, and2753c may function as a cathode electrode contact.
Alternatively, electrode2750 may be utilized to reduce muscle fatigue when implanted on single function nerves, such as, for example, the hypoglossal nerve. In such circumstances, muscle fatigue may be reduced by alternatively switching between using loosely spaced electrode contacts2753a,2753c, and2753e, to stimulate large diameter fibers, and closely spaced electrode contacts2753a-2753e, to stimulate small diameter fibers.
Turning toFIGS. 27J-27K, in accordance with the present disclosure, there is depicted another embodiment of a nerve cuff electrode2760 for facilitating reduction in muscle fatigue. Nerve cuff electrode2760 may include abody2761 having a plurality ofelectrode contacts2762,2763, and2764. Electrode contacts2762-2764 may include any suitable electrode contacts in accordance with the present disclosure. Although the depicted embodiment of nerve cuff electrode2760 includes three electrode contacts2762-2764, nerve cuff electrode2760 may include a greater or lesser number of electrode contacts. Furthermore, electrode contacts may be disposed onbody2761 in any suitable configuration to achieve the desired effect, such as, for example, serially, as depicted. In the depicted embodiment,electrode contacts2762 and2764 may function as anode electrode contacts, whileelectrode contact2763 may function as a cathode electrode contact.Electrode contact2763 may include two distinct, substantially triangularly shaped portions2763a and2763b. However, portions2763a and2763b may include any suitable shape. In addition, portions2763a and2763b may be configured to be of differing conductive properties, so that, for the same stimulation pulse (e.g., a slow rising, small amplitude pulse having a relatively long duration of approximately 0.2 to 0.35 milliseconds) applied to each of the portions2763a and2763b, the resultant charge densities at the surface of each of the portions2763a and2763b may be different. For example, portions2763a and2763b may be made of electrically differing materials. For discussion purposes only, it is assumed that portion2763a is configured to deliver a charge density lower than that of portion2763b. However, portion2763a may be configured to deliver a charge density that is higher than the charge density of portion2763b.
Since the small diameter fibers of a nerve are typically stimulated by low charge densities and large diameter fibers of the nerve are typically stimulated by high charge densities, portions2763a and2763b may be sequentially utilized to alternate between stimulating the small and large diameter fibers of a nerve. In other words, in use, a stimulation pulse may be first delivered to portion2763a to stimulate the small diameter fibers of a nerve. A subsequent stimulation pulse may be then delivered to portion2763b to stimulate the large diameter fibers of a nerve. It is contemplated that alternating between stimulating the small and large diameter fibers of a nerve may facilitate reducing muscle fatigue while also ensuring sufficient muscle mass is stimulated to maintain the necessary contraction and force generation to successfully treat OSA.
Turning now toFIG. 27L, there is illustrated yet another embodiment of anerve cuff electrode2780 for facilitating reduction in muscle fatigue. For the purposes of this disclosure,nerve cuff electrode2780 may be substantially similar to nerve cuff electrode2760.Nerve cuff electrode2780, however, may differ from nerve cuff electrode2760 in at least one significant way. For example, rather than having two substantially triangular portions,cathode electrode contact2783 may comprise two substantially different portions2783a and2783b. Portions2783a and27836 may be spaced apart from one another and may include differing surface areas. For example, as illustrated, portion2783a may include a smaller surface area than portion2783b. Furthermore, portions2783a and2783b may include any suitable shape known in the art. Although portions2783a and2783b in the illustrated embodiment together define a substantially triangular shapedelectrode contact2783, portions2783a and2783b together may or may not define any suitable shape known in the art.
Each of portions2783a and2783b may be configured to be substantially similar in conductance despite their differing surface areas. For example, portion2783a may be made of a first material having a relatively lower conductance, while portion2783b may be made of a second material having a relatively higher conductance. Thus, when subjected to the same stimulation pulse (e.g., a slow rising, small amplitude pulse having a relatively long duration of approximately 0.2 to 0.35 milliseconds), portion2783a may have a higher charge density than portion2783b because of its relatively smaller surface area than portion2783b. Similarly, when subjected to the same stimulation pulse, portion2783b may have a lower charge density than portion2783a because of its relatively larger surface area than portion2783a. Accordingly, because of the differing charge densities, portion2783a may be adapted to stimulate large diameter fibers of a nerve, and portion2783b may be adapted to stimulate small diameter fibers of the nerve.
In use, a stimulation pulse may be first delivered to portion2783a to stimulate the large diameter fibers of a nerve. A subsequent stimulation pulse may be then delivered to portion2783b to stimulate the small diameter fibers of the nerve. It is contemplated that alternating between stimulating the small and large diameter fibers of a nerve may facilitate muscle fatigue while also ensuring that sufficient muscle mass is stimulated to maintain the necessary contraction and force generation to successfully treat OSA.
In certain embodiments, such as whennerve cuff electrodes2760 and2780 are implanted on a multi-function nerve (e.g., the superior laryngeal nerve SLN), it is contemplated that portions2763a/2763b and portions2783a/2783b may be utilized to selectively stimulate either the afferent or efferent fibers of the nerve.
With reference now toFIGS. 27M-27Q, there is depicted yet another embodiment of anerve cuff electrode2790 for minimizing muscle fatigue.Nerve cuff electrode2790 may include acuff body2791 for mounting about anerve2792 in accordance with the present disclosure.Cuff body2791 may include a plurality of electrode contacts2793-2796 also in accordance with the present disclosure. Although the depicted embodiment ofnerve cuff electrode2790 includes four electrode contacts2793-2796,nerve cuff electrode2790 may include a greater or lesser number of electrode contacts.
Nerve cuff electrode2790 may be configured to selectively stimulate both small diameter fibers contained infascicle2777a and large diameter fibers contained infascicle2777b ofnerve2792. For example, as shown inFIG. 27P, by applying an exemplary slow rising, long pulse width waveform toelectrode contacts2796 and2793,nerve cuff electrode2790 may stimulate the small diameter fibers contained infascicle2777a ofnerve2792. Similarly, as shown inFIG. 27Q, by applying an exemplary fast rising, short pulse width waveform toelectrode contacts2794 and2795,nerve cuff electrode2790 may stimulate the large diameter fibers contained infascicle2777b ofnerve2792.Fascicles2777a and2777b may be stimulated simultaneously or separately. In embodiments, where it is desirable to stimulate fibers contained infascicles2777a and2777b, the pulse generator (e.g., INS50) may be provided with dual output ports.
Description of Respiration Sensing Lead Anchoring Alternatives
With reference to the following figures, various additional or alternative anchoring features for therespiration sensing lead70 are schematically illustrated. Anchoring therespiration sensing lead70 reduces motion artifact in the respiration signal and stabilizes the bio-impedance vector relative to the anatomy.
In each of the embodiments, by way of example, not limitation, therespiration sensing lead70 includes alead body70 with a proximal connector and a plurality ofdistal respiration sensors74 comprising ring electrodes for sensing bio-impedance. Thelead body72 of therespiration sensing lead70 may include a jacket cover containing a plurality ofconductors78, one for eachring electrode74 requiring independent control. Generally, theimpedance electrodes74 may comprise current emitting electrodes and voltage sensing electrodes for detecting respiration by changes in bio-impedance.
With reference toFIGS. 28-33, various fixation devices and methods are shown to acutely and/or chronically stabilize therespiratory sensing lead70. With specific reference toFIG. 28, theINS50 is shown in a subcutaneous pocket and thestimulation lead60 is shown in a subcutaneous tunnel extending superiorly from the pocket. Therespiration sensing lead70 is shown in a subcutaneous tunnel superficial to muscle fascia around the rib cage. A suture tab or ring270 may be formed with or otherwise connected to the distal end of thelead body72. Near the distal end of thelead70, a small surgical incision may be formed to provide access to the suture tab270 and the muscle fascia under thelead70. The suture tab270 allows the distal end of thelead70 to be secured to the underlying muscle fascia by suture orstaple272, for example, which may be dissolvable or permanent. Both dissolvable and permanent sutures/staples provide for acute stability and fixation until thelead body72 is encapsulated. Permanent sutures/staples provide for chronic stability and fixation beyond what tissue encapsulation otherwise provides.
With reference toFIGS. 29A-29C, afabric tab280 may be used in place of or in addition to suture tab270. As seen inFIG. 29A, thefabric tab280 may be placed over a distal portion of thelead body72, such as between twodistal electrodes74. A small surgical incision may be formed proximate the distal end of thelead70 and thefabric tab280 may be placed over the over thelead body72 and secured to the underlying muscle fascia by suture orstaple282, for example, which may be dissolvable or permanent, to provide acute and/or chronic stability and fixation. With reference toFIGS. 29B and 29C (cross-sectional view taken along line A-A), thefabric tab280 may comprise a fabric layer (e.g., polyester)284 to promote chronic tissue in-growth to the muscle fascia and a smooth flexible outer layer (silicone or polyurethane)286 for acute connection by suture orstaple282.
With reference toFIG. 30, lead70 includes a split ring290 that may be formed with or otherwise connected to the distal end of thelead body72. The split ring290 allows the distal end of thelead70 to be secured to the underlying muscle fascia by suture orstaple292, for example, which may be dissolvable or permanent. The ring290 may be formed of compliant material (e.g., silicone or polyurethane) and may include a slit294 (normally closed) that allows thelead70 to be explanted by pulling thelead70 and allowing thesuture292 to slip through the slit294, or if used without a suture, to allow the ring to deform and slide through the tissue encapsulation. To further facilitate explanation, adissolvable fabric tab282 may be used to acutely stabilize thelead70 but allow chronic removal.
With reference toFIGS. 31A-31C,deployable anchor tines300 may be used to facilitate fixation of thelead70. As seen inFIG. 31A, the self-expandingtines300 may be molded integrally with thelead body72 or connected thereto by over-molding, for example. Thetines300 may comprise relatively resilient soft material such as silicone or polyurethane. Theresilient tines300 allow thelead70 to be delivered via a tubular sheath ortrocar304 tunneled to the target sensing site, wherein thetines300 assume a first collapsed delivery configuration and a second expanded deployed configuration. As seen inFIGS. 31B and 31B′, the tubular sheath or trocar301 may be initially tunneled to the target site using anobturator306 with ablunt dissection tip308. After the distal end of thetubular sheath304 has been tunneled into position by blunt dissection using theobtruator306, theobtruator306 may be removed proximally from thesheath304 and thelead70 withcollapsible tines300 may be inserted therein. As seen inFIG. 31C, when the distal end of thelead70 is in the desired position, thesheath304 may be proximally retracted to deploy thetines300 to engage the muscle fascia and adjacent subcutaneous tissue, thus anchoring thelead70 in place.
With reference toFIGS. 32A and 32B, an alternative deployable fixation embodiment is shown schematically. In this embodiment, self-expandingtines310 are held in a collapsed configuration byretention wire312 disposed in the lumen of thelead body72 as shown inFIG. 32A. Each of thetines310 includes ahole314 through which theretention wire312 passes to hold thetines310 in a first collapsed delivery configuration as shown InFIG. 32A, and proximal withdrawal of theretention wire314 releases theresilient tines310 to a second expanded deployed configuration as shown inFIG. 32B. Thelead70 may be tunneled to the desired target site with thetines310 in the collapsed configuration. Once in position, thewire312 may be pulled proximally to release thetines310 and secure thelead70 to the underlying muscle fascia and adjacent subcutaneous tissue to establish fixation thereof.
With reference toFIGS. 33A and 33B, another alternative deployable fixation embodiment is shown schematically. In this embodiment, self-expanding structures such as one or moreresilient protrusions320 and/or a resilient mesh325 may be incorporated (either alone or in combination) into the distal end of thelead70. By way of example, not limitation,resilient protrusions320 may comprise silicone or polyurethane loops and resilient mesh325 may comprise a polyester fabric connected to or formed integrally with thelead body72. Both theresilient protrusions320 and the resilient mesh325 may be delivered in a collapsed delivery configuration insidetubular sheath304 as shown inFIG. 33A, and deployed at the desired target site by proximal retraction of thesheath304 to release the self-expandingstructures320/325 to an expanded deployed configuration as shown inFIG. 33B. Both theresilient protrusions320 and the resilient mesh325 engage the underlying muscle fascia through tissue encapsulation and adjacent subcutaneous tissues to provide fixation of thelead70 thereto.
Other fixation embodiments may be used as well. For example, the fixation element may engage the muscle fascia and adjacent subcutaneous tissues or may be embedded therein. To this end, the electrodes may alternatively comprise intramuscular electrodes such as barbs or helical screws.
Description of Respiration Sensing Electrode Alternatives
A description of the various alternatives in number, spacing, anatomical location and function of the impedance electrodes follows. Generally, in each of the following embodiments, the respiration sensing lead includes a lead body and a plurality of respiration sensors comprising ring electrodes for sensing bio-impedance. The lead body may include a plurality of insulated conductors disposed therein, with one conductor provided for each ring electrode requiring independent connection and/or control. The impedance electrodes may comprise current emitting electrodes and voltage sensing electrodes for detecting respiration by changes in bio-impedance.
With reference toFIG. 34, the distal portion of arespiration sensing lead70 is shown by way of example, not limitation. Therespiration sensing lead70 includes alead body72 with a proximal connector and a plurality ofdistal impedance electrodes74. In this example, thelead body72 andelectrodes74 are cylindrical with a diameter of 0.050 inches. The distal current-carrying electrode74A may be 5 mm long and may be separated from the voltage-sensing electrode74B by 15 mm. The distal voltage sensing electrode may be 5 mm long and may be separated from the proximal combination current-carrying voltage-sensing electrode74C by 100 mm. The proximal electrode74C may be 10 mm long. The proximal portion of thelead70 is not shown, but would be connected to the INS (not shown) as described previously. The lead body incorporates a plurality of insulated electrical conductors (not shown), each of which correspond to an electrode74A-74C. The electrodes and conductors may be made of an alloy of platinum-iridium. Thelead body72 may comprise a tubular extrusion of polyurethane, silicone, or a coextrusion of polyurethane over silicone. The conductors may be formed of multi-filar wire coiled to provide extensibility for comfort and durability under high-cycle fatigue.
With reference toFIGS. 35A-35E, the position of theelectrodes74 may be characterized in terms of bio-impedance or bio-Z vectors. The bio-Z vector may be defined by the locations of the voltage-sensing electrodes (labeled V1& V2). The voltage-sensing electrodes may be located on either side of the current-carrying electrodes (labeled I1& I2). For example, it is possible to locate either one or both of the voltage-sensing electrodes between the current-carrying electrodes as shown inFIG. 35A (4-wire configuration (I1-V1-V2-I2)), and it is possible to locate either one or both of the current-carrying electrodes between the voltage-sensing electrodes as shown inFIG. 35B (inverted 4-wire configuration (V1-I1-I2-V2)). While at least two separate electrodes (I1& I2) are required to carry current and at least two separate electrodes (V1& V2) are required to measure voltage, it is possible to combine the current carrying and voltage sensing functions in a common electrode. Examples of combining voltage sensing and current carrying electrodes are shown inFIGS. 35C-35E.FIG. 35C (2-wire configuration (I1V1-I2V2)) shows combination electrode I1V1and I2V2where each of these electrodes is used to carry current and sense voltage.FIG. 35D (3-wire configuration (I1-V1-I2V2)) and35E (inverted 3-wire configuration (V1-I1-I2V2)) show combination electrode I2V2which is used to carry current and sense voltage.
With reference toFIG. 36, insulative material such as strips73 may cover one side of one or more electrodes74A-74D to provide directional current-carrying and/or voltage-sensing. The insulative strips may comprise a polymeric coating (e.g., adhesive) and may be arranged to face outward (toward the dermis) such that the exposed conductive side of eachelectrode74 faces inward (toward the muscle fascia and thoracic cavity). Other examples of directional electrodes would be substantially two-dimensional electrodes such as discs or paddles which are conductive on only one side. Another example of a directional electrode would be a substantially cylindrical electrode which is held in a particular orientation by sutures or sutured wings. Another example of a directional electrode would be an electrode on the face or header of the implanted pulse generator. It would likely be desirable for the pulse generator to have a non-conductive surface surrounding the location of the electrode.
In addition to the cylindrical electrodes shown, other electrode configurations are possible as well. For example, the electrodes may be bi-directional with one planar electrode surface separated from another planar electrode surface by insulative material. Alternatively or in combination, circular hoop electrodes may be placed concentrically on a planar insulative surface. To mitigate edge effects, each electrode may comprise a center primary electrode with two secondary side electrodes separated by resistive elements and arranged in series. An alternative is to have each primary current-carrying electrode connected by a resistive element to a single secondary side electrode. The conductive housing of theINS50 may serve as an current-carrying electrode or voltage-sensing electrode. Alternatively or in addition, an electrode may be mounted to the housing of theINS50.
Because bio-impedance has both a real and imaginary component, it is possible to measure the bio-Z phase as well as magnitude. It may be preferable to extract both magnitude and phase information from the bio-Z measurement because the movement of the lung-diaphragm-liver interface causes a significant change in the phase angle of the measured impedance. This may be valuable because motion artifacts of other tissue have less impact on the bio-Z phase angle than they do on the bio-Z magnitude. This means the bio-Z phase angle is a relatively robust measure of diaphragm movement even during motion artifacts.
An example of a bio-Z signal source is a modulated constant-current pulse train. The modulation may be such that it does not interfere with the stimulation signal. For example, if the stimulation signal is 30 Hz, the bio-Z signal source signal may be modulated at 30 Hz or a sub-multiple of 30 Hz such that bio-Z and stimulation do not occur simultaneously. The pulses in the pulse train may have a pulse width between 1 uS to 1 mS, such as 100 uS. The pulses may be separated by a period of time roughly equal to the pulse width (i.e., on-time of the pulses). The number of pulses in a train may be determined by a trade-off between signal-to-noise and power consumption. For example, no more than 10 pulses may be necessary in any given pulse train. The magnitude of current delivered during the pulse on-time may be between 10 uA and 500 uA, such as 50 uA.
Other wave forms of bio-Z source signal may be used, including, without limitation, pulse, pulse train, bi-phasic pulse, bi-phasic pulse train, sinusoidal, sinusoidal w/ramping, square wave, and square w/ ramping. The bio-Z source signal may be constant current or non-constant current, such as a voltage source, for example. If a non-constant current source is used, the delivered current may be monitored to calculate the impedance value. The current-carrying electrodes may have a single current source, a split-current source (one current source split between two or more current-carrying electrodes), or a current mirror source (one current source that maintains set current levels to two or more current-carrying electrodes). Different characteristics of the sensed signal may be measured including, without limitation, magnitude, phase shift of sensed voltage relative to the current source signal, and multi-frequency magnitude and/or phase shift of the sensed signal. Multi-frequency information may be obtained by applying multiple signal sources at different frequencies or a single signal source which contains two or more frequency components. One example of a single multifrequency source signal is a square wave current pulse. The resultant voltage waveform would contain the same frequency components as the square wave current pulse which would allow extraction of Bio-Z data for more than a single frequency.
With reference toFIG. 37, the bio-Z vector may be oriented with regard to the anatomy in a number of different ways. For example, using the electrode arrangement illustrated inFIG. 34 and the anatomical illustration inFIG. 37, the bio-Z vector may be arranged such that the proximal combination electrode is located just to the right of and above the xiphoid below the pectoral muscle between the 5thand 6thribs and the distal current-carrying electrode is located mid-lateral between the 7thand 8thribs, with the distal voltage-sensing electrode positioned between the 6thand 7thribs 10 mm proximal of the distal current-carrying electrode. This arrangement places the electrodes along the interface between the right lung, diaphragm and liver on the right side of the thoracic cavity. The lung-diaphragm-liver interface moves relative to the bio-Z vector with every respiratory cycle. Because the lung has relatively high impedance when inflated and the liver has relatively low impedance due to the conductivity of blood therein, this bio-Z vector arrangement across the lung-diaphragm-liver interface provides for a strong respiratory signal that is indicative of changes between inspiration and expiration. In addition, because the heart is situated more on the left side, positioning the bio-Z vector on the right side reduces cardiac artifact. The net result is a bio-Z vector that provides an excellent signal-to-noise ratio.
A variety of different bio-Z vector orientations relative to the anatomy may be employed. Generally, bio-Z vectors for monitoring respiration may be located on the thorax. However, bio-Z electrodes located in the head and neck may also be used to define respiratory bio-Z vectors. By way of example, not limitation, the bio-Z vector may be arranged transthoracically (e.g., bilaterally across the thorax), anteriorly on the thorax (e.g., bilaterally across the thoracic midline), across the lung-diaphragm-liver interface, perpendicular to intercostal muscles, between adjacent ribs, etc. A single bio-Z vector may be used, or multiple independent vectors may be used, potentially necessitating multiple sensing leads. One or more bio-Z sub-vectors within a given bio-Z vector may be used as well.
With reference toFIGS. 37A-37C, thoracic locations defining examples of bio-Z vectors are shown schematically.FIG. 37A is a frontal view of the thorax,FIG. 37B is a right-side view of the thorax, andFIG. 37C is a left-side view of the thorax. In each ofFIGS. 37A-37C, the outline of the lungs and upper profile of the diaphragm are shown. As mentioned previously, a bio-Z vector may be defined by the locations of the voltage-sensing electrodes. Thus,FIGS. 37A-37C show locations for voltage sensing electrodes which would define the bio-Z vector.
There are several short bio-Z vectors which provide excellent signals correlated to diaphragmatic movement. In general, these vectors have at least one end at or near the lower edge of the ribcage. The short diaphragmatic bio-Z vectors have been successfully used in canines in vector lengths ranging from approximately less than ½ inch to a few inches in length.FIG. 37A shows a variety of locations which are representative of the locations which define such vectors. Locations shown just below the ribcage on the person's right side are designated as A, B, C, and D. Locations shown just below the ribcage on the person's left side are E, F, G, and H. Locations shown just above the lower edge of the ribcage on the person's right side are I, J, K, and L. Locations shown just above the lower edge of the ribcage on the person's left side are M, N, P, and Q. The locations just above the lower edge of the ribcage would fall within a few inches of the lower edge. Short diaphragmatic monitoring vectors would be comprised of location pairs which are relatively closely spaced. For example, vectors D-E, D-C, D-L, and D-K all provide good diaphragmatic signal. The possible vectors fall into three groups. Exemplary vectors which measure primarily diaphragmatic muscle contraction are A-B, B-C, C-D, D-E, E-F, F-G, and G-H. Exemplary vectors which measure a combination of diaphragmatic muscle contraction combined with movement of the lung into the pleural pocket as the diaphragm contracts are I-J, P-R, A-I, A-J, B-I, B-J, G-P, H-R, H-P, and G-R. Exemplary vectors which measure diaphragmatic muscle contraction combined with movement of the diaphragm away from the thoracic wall as that portion of the lung expands are J-K, K-L, M-N, and N-P. It is known that the signal from any given location may be affected by body position and free vs. obstructed respiration. The respiratory signal from short vectors at or near the lower edge of the ribcage may be more robust (e.g., may be not be substantially affected) to body position and obstructed respiration. A further means of obtaining a signal which may be also more robust to body position would be to measure the respiratory impedance from complimentary vectors and sum the resulting bio-Z measurements. Complimentary vectors would be mirror-images or nearly mirror images of one another. Examples of vectors and their mirror images may be C-D and E-F, B-C and G-F, C-K and F-N.
By way of example, not limitation, the following bio-Z vectors may be effective for monitoring respiration and/or for measuring artifacts for subsequent removal of the artifact from the respiration signal. Vector C-G is across the upper left and upper right lobes of the lungs, and provides a good signal of ribcage expansion with moderate cardiac artifact. Vector D-F is a short-path version of C-G that provides a good respiratory signature largely correlated with ribcage expansion, with less cardiac artifact than C-G, but may be sensitive to movement of arms due to location on pectoral muscles. Vector C-D is a short-path ipsilateral vector of the upper right lung that may be sensitive to arm movement but has less cardiac artifact. Vector B-H is a transverse vector of the thoracic cavity that captures the bulk of the lungs and diaphragm movement. Vector B-H, however, may be relatively less susceptible to changes in body position, and may still provide a generally good signal when the patient changes positions. In certain circumstances, the signal produced by vector B-H may have a less than desired signal to noise ratio. However, it is contemplated that generally available methods of signal processing in accordance with the present disclosure may be utilized the improve signal to noise ratio of the signal produced by Vector B-H. Vector A-E is an ipsilateral vector across the lung-diaphragm-liver interface. Because the liver is higher in conductivity and has a different impedance phase angle than the lung, vector A-E1 yields a good signal on both bio-Z magnitude and phase with limited cardiac artifact. Vector B-K is an ipsilateral vector across the lung-diaphragm-liver interface that is substantially between a common set of ribs with a current path that is mostly perpendicular to the intercostal muscles. Because resistivity of muscle is much higher perpendicular to the muscle direction than parallel, vector B-K reduces current-shunting through the muscle which otherwise detracts from the signal of the lung-diaphragm-liver interface. Vector A-K is an ipsilateral vector across the lung-diaphragm-liver interface similar tovector A-E1 but is more sensitive to movement of the lung-diaphragm-liver interface than to changes in resistivity of the lung-diaphragm-liver interface due to inspired air volume and is thus a good indicator of diaphragm movement.Vector B-E1 is a vector across the middle and lower right lung and is good for detecting diaphragm movement with little cardiac artifact.Vector C-E1 is a vector across the upper and middle right lung and is also good for detecting diaphragm movement with little cardiac artifact.Vector D-E1 is a vector across the upper right lung with little cardiac artifact. Vector A-D is an ipsilateral across a substantial portion of the right lung and diaphragm with little cardiac artifact, but may be susceptible to motion artifact due to arm movement. Vector E1-E2 is a vector across the heart and provides a good cardiac signal that may be used for removing cardiac artifact from a respiratory signal. Vector E2-J is a vector across the lung-diaphragm-stomach interface that provides a good measure of diaphragm movement using bio-Z phase vs. magnitude because the stomach has almost no capacitive component and generally low conductivity. Vector L-M is a trans-diaphragm vector that is generally across the lung-diaphragm-liver interface with little cardiac artifact. Vector L-M may be relatively less susceptible to body position and movement and may yield a good signal even if the patient is laying on the side of the sensing lead. In embodiments where the signal produced by vector L-M has a less than desired signal to noise ratio, it is contemplated that generally available methods of signal processing may be utilized to improve the signal to noise ratio of the signal produced by vector L-M.
Electrodes placed at any of the above-noted locations may include, but are not limited to, combination electrodes, such as, for example, electrodes capable of both providing a current charge and sensing a voltage.
With reference toFIGS. 37A and 38D, an exemplary vector selection method3800 for detecting and utilizing a signal from the vector that produces the most desirable signal of all vectors is discussed. The disclosed vector selection method3800 may be performed continuously, periodically, singularly, and/or may be repeated as desired. For example, method3800 may be performed once in a 24 hour period. In addition, one or more steps associated with method3800 may be selectively omitted and/or the steps associated with method3800 may be performed in any order. The steps associated with method3800 are described in a particular sequence for exemplary purposes only.
With specific reference toFIG. 38D, method3800 may include a plurality of steps3801-3803 for detecting and utilizing the signal with the best characteristics of all signals produced by a plurality of vectors. Specifically, method3800 may include sampling short distance vectors first to determine if any of these vectors are producing a desirable signal,step3801. Method3800 may also include sampling intermediate distance vectors if the short distance vectors are not producing a desirable signal,step3802. Method3800 may further include sampling long distance vectors if the intermediate distance vectors are not producing a desirable signal, isstep3803.
Turning toFIG. 37A, there is depicted an exemplary embodiment of a neurostimulator in accordance with the principles of the present disclosure. The exemplary neurostimulator may include an implantedINS50 and implanted electrode contacts AA-DD. While the depicted embodiment includes electrode contacts AA-DD disposed between a patient's 5thand lowest ribs, electrode contacts AA-DD may be disposed at any suitable location. Furthermore, electrode contacts AA-DD may include, but are not limited to, the combination electrodes discussed above. In the depicted embodiment, exemplary short distance vectors may include the vectors between, for example, adjacent electrode contacts AA, BB, CC, and DD; exemplary intermediate distance vectors may include the vectors AA-CC, AA-DD, and BB-DD, and exemplary long distance vectors may include the vectors between theINS50 and each of electrode contacts AA-DD.
With reference toFIG. 37A andFIG. 38A,step3801 may include, for example, sampling short distance vectors AA-BB, BB-CC, and CC-DD first to determine whether any of these vectors may be producing a sufficient signal in accordance with the principles of this disclosure, since these vectors generally produce signals with desirable signal to noise ratios. Next,step3802 of method3800 may include sampling the intermediate distance vectors AA-CC, AA-DD, and BB-DD if the short distance vectors are producing a less than desirable signal. Lastly,step3803 of method3800 may include sampling the long distance vectors INS-AA, INS-BB, INS-CC, and INS-DD if the intermediate distance vectors are producing a less than desirable signal.
In some embodiments, it is contemplated that several short, intermediate, and long distance vectors may be continually sampled, even if a desirable signal is being received from a short distance vector, in order to identify secondary vector signals that may be utilized if the currently utilized vector signal fails for any reason. However, fully processing the data from signals generated by all of the vectors may require complex sensing circuitry and processing of detection algorithms that may utilize undesirable amounts of battery power. Therefore, it may be desirable to only monitor selected characteristics of the secondary vector signals. With specific reference toFIG. 38B, there is depicted an embodiment of a method3850 for utilizing multiple sensing channels to optimize respiratory sensing with minimal additional hardware and power consumption. It uses a single sensing circuit which is time multiplexed (interleaved) to sample each of the vectors. Since, as noted above, fully processing the data from all vector signals may require higher computational power, method3850 may be used to identify the best vector signal for respiration detection, while simultaneously monitoring the remaining vectors signals for only relevant fiducial points. These fiducial points may include, but are not limited to, significant “landmarks” within a signal, such as, for example, peak amplitude and time, point of highest slew rate, and zero crossing. The detected fiducial points for the secondary vector signals may be then stored in acircular buffer memory3854 for analysis if the primary signal fails for any reason, thereby, allowing immediate switching to an alternate vector signal and eliminating the need for a long signal acquisition period after a need to switch vector signals has been determined.
In particular, method3850 may include feeding the signals from all available vectors into a plurality of channel selection switches3851. The signals may be then analyzed for relevant fiducials by the respiratoryimpedance sensing circuit3853. Once relevant fiducials have been discriminated, it may be possible to identify the best vector signal for respiration signal analysis. The fiducials of the remaining vectors may be then stored in circular buffer memory3854 (as noted above) to facilitate switching to a secondary vector signal if the primary signal is no longer suitable for respiration detection.
The periodic monitoring (or interleaving) of secondary vector signals may facilitate faster switching to those vector signals when necessary. In particular, it is contemplated that when a decision to switch to a secondary vector signal is made (i.e., when the primary signals degrades to a point where it is no loner desirable for detecting respiration), the saved data (e.g., relevant fiducials) may be used to “seed” a signal analysis algorithm with recently collected data, so as to promote faster vector switching by eliminating the need to wait for collection of sufficient data for the secondary vector signal. In other words, because select information of a secondary signal is available before the signal is actually used for respiration detection, analysis of the secondary signal for, among other things, respiration detection may begin slightly faster than it would have if no data was available.
Furthermore, in certain embodiments, additional impedance sensors may be used as backup sensors to the sensor generating the primary vector signal. In these embodiments, data from the secondary sensors may be also analyzed to identify and save relevant fiducials in the memory. This stored information may be used to provide supplemental or alternate information to facilitate identifying appropriate respiratory timing, when switching vector signals becomes necessary as a result of primary signal degradation.
The respiratory bio-Z signal is partly due to the resistivity change which occurs when air infuses lung tissue, partly due to the relative movement of electrodes as the rib cage expands, and partly due to the displacement of other body fluids, tissue and organs as the lungs move along with the ribcage and diaphragm. As described above, each vector measures certain of these changes to different extents. It may be desirable, therefore, to combine vectors which have complementary information or even redundant information to improve the respiratory information of the bio-Z signal. To this end, multiple vectors may be used. For example, one vector may be used to sense changes in the lung-diaphragm-liver interface and a second vector may be used to detect changes (e.g., expansion, contraction) of the lung(s). Examples of the former include A-K, B-K,A-E1,B-E1, and A-B. Examples of the later include D-F, B-D, C-G,D-E1, andC-E1. Note that some vector combinations which share a common vector endpoint such asA-E1,D-E1 andB-E1, B-D may use a common electrode which would simplify the respiratory sensing lead or leads.
An advantage of using the lung-diaphragm-liver interface vector is that it provides a robust signal indicative of the movement of the diaphragm throughout the respiratory cycle. The liver is almost two times more electrically conductive than lung tissue so a relatively large bio-Z signal can be obtained by monitoring the movement of the lung-diaphragm-liver interface. Because the liver functions to filter all the blood in the body, the liver is nearly completely infused with blood. This helps to dampen out the cardiac artifact associated with the pulsatile flow of the circulatory system. Another advantage of this location is that vectors can be selected which avoid significant current path through the heart or major arteries which will help reduce cardiac artifact.
It is worth noting that diaphragm movement is not necessarily synchronous with inspiration or expiration. Diaphragm movement typically causes and therefore precedes inspiration and expiration. Respiratory mechanics do allow for paradoxical motion of the ribcage and diaphragm, so diaphragm movement is not necessarily coincident with inspiration. During REM sleep, the diaphragm is the dominant respiratory driver and paradoxical motion of the ribs and diaphragm can be problematic, especially if movement of the ribcage is being relied upon as an inspiratory indicator. Monitoring the diaphragm for pre-inspiratory movement becomes especially valuable under these circumstances. Bio-Z monitoring of the diaphragm can be used as a more sophisticated indicator of impending inspiration rather than the antiquated approach of desperately trying to identify and respond to inspiration in pseudo-real time based on sensors which are responding to characteristics of inspiration.
For purposes of monitoring respiration, it is desirable to minimize shunting of the electrical current through tissues which are not of interest. Shunting may result in at least two problems: reduced signal from the lungs; and increased chance of artifacts from the shunted current path. Skeletal muscle has non-isotropic conductivity. The muscle's transverse resistivity (1600 ohm-cm) is more than 5 times its longitudinal resistivity (300 ohm-cm). In order to minimize the adverse effect of shunting current, it is desirable to select bio-Z sensing vectors which are perpendicular to muscle structure if possible. One such example is to locate two or more electrodes of a bio-Z sensing array substantially aligned with the ribs because the intercostal muscles are substantially perpendicular to the ribs.
Description of Respiration Signal Processing
With reference toFIG. 39, the neurostimulation system described herein may operate in a closed-loop process400 wherein stimulation of the targeted nerve may be delivered as a function of a sensed feedback parameter (e.g., respiration). For example, stimulation of the hypoglossal nerve may be triggered to occur during the inspiratory phase of respiration. Alternatively, the neurostimulation system described herein may operate in an open-loop process wherein stimulation is delivered as a function of preset conditions (e.g., historical average of sleeping respiratory rate).
With continued reference toFIG. 39, the closed-loop process400 may involve a number of generalized steps to condition the sensed feedback parameter (e.g., bio-Z) into a useable trigger signal for stimulation. For example, the closed-loop process400 may include the initial step of sensingrespiration350 using bio-Z, for example, and optionally sensingother parameters360 indicative of respiration or other physiologic process. The sensed signal indicative of respiration (or other parameter) may be signal processed370 to derive a usable signal and desired fiducials. A trigger algorithm380, which will be discussed in greater detail below, may then be applied to the processed signal to control delivery of thestimulation signal390.
As noted above, the present disclosure contemplates conditioning sensed bio-impedance into a useable trigger signal for stimulation. However, one exemplary limitation to using sensed bio-impedance may be the body's nominal impedance. In practice, a sensed bio-impedance signal may be obtained by applying a suitable, known current through one portion of a tissue of interest and measuring the voltage potential across the same tissue. This measurement technique is illustrated inFIG. 38C and may be referred to herein as the “direct measurement” technique. The applied current and measured voltage potentials may be used to calculate the impedance of the tissue. It is this measured impedance that may constitute the sensed bio-impedance signal. However, sense bio-impedance signals of the present disclosure have been found to typically include two components, a relatively large nominal body impedance component and a relatively small respiratory impedance component. Thus, since the body's impedance constitutes a large portion of the sensed signal, it may be difficult to detect that relatively small impedance changes associated with respiration on top of a body's nominal impedance. Therefore, in accordance with the principles of the present disclosure, it may be desirable to “filter” the sensed impedance signal in a manner so as to remove most or all of the body's nominal impedance, in order to improve resolution of the respiratory signal. In some embodiments, this may be achieved with the aid of a conventional Wheatstone bridge at or near the front-end of an impedance measuring circuit. In particular, the Wheatstone bridge may facilitate precise measurements of the relatively small impedance changes associated with respiration by removing most, if not all, of the body's nominal impedance.
Turning now toFIG. 39A, there is depicted an exemplary Wheatstone bridge3900. The Wheatstone bridge3900 may include an electricalcurrent source3901. Wheatstone bridge3900 may also include a first resistor R1having an impedance Z1connected in series to a second resistor R2having an impedance Z2. Resistors R1and R2may be connected in parallel to resistor R3having an impedance Z3, which may be connected serially to the patient's body having an impedance Zbody. As discussed below, impedances Z2and Z3may be substantially similar to each other. Wheatstone bridge3900 may further include any suitable voltage measuring device, such as, for example, those used in conjunction the direct measurement technique described above.
In use, the impedance Z1of exemplary bridge3900 may be closely matched to the expected impedance of a patient's body Zbody, the impedance Z2matched to impedance Z3, and the voltage potential across voltage measuring device3902 may be measured. It is contemplated that if impedances Z1-Z3are closely matched to Zbody, the measured voltage potential across voltage measuring device3902 will be predominantly due to respiratory impedance changes and the voltage signal due to the body's nominal impedance will be largely removed. Further, it is contemplated that the voltage changes measured at3902 due to respiratory impedance changes will have an amplitude that is approximately ½ of the amplitude of the voltage changes, measured with the above-noted direct-measurement technique, assuming the same currently flow through the body. The removal of the voltage signal due to the body's nominal impedance while retaining ½ of the voltage signal amplitude due to changes in respiratory impedance, may facilitate detecting the small impedance changes associated with respiration by improving the resolution of those changes.
In other embodiments, the body's nominal impedance may be extracted and identified (e.g., type, time, and value). be removed or reduced from a sensed signal by, for example, introducing a nominal offset removal module3921 into animpedance measuring circuit3920 of the present disclosure, as depicted inFIG. 39B. An exemplary impedance-measuring circuit may generally include feeding a sensed respiratory signal into a demodulator. The signal exiting the demodulator may be then fed into an integrator, and the integrated signal exiting the integrator may then be digitized for analysis. It is therefore contemplated that introducing nominal offset removal module3921 to act upon the upon the signal exiting the demodulator may achieve the desired effect of removing or reducing the body's nominal impedance from a sensed impedance signal.
Turning now toFIG. 39C, module3921 may include a switch S, a resistor R, a capacitor C, and a non-inverting amplifier A. The switch S, resistor R, and capacitor C create a sample and hold reference voltage to the difference amplifier A. The amplifier subtracts this reference voltage from the input signal. The result is to remove or reduce the nominal body impedance component of the signal leaving mainly the respiratory component of the measured impedance. The Resistor-Capacitor (R-C) combination is selected such that it will track with changes in nominal impedance levels but does not significantly distort the respiratory signal. Respiratory signal frequency components of interest are typically between 0.05 Hz and 3 Hz. There are several options for how the Nominal Offset Removal may be operated. An implanted bio-impedance circuit would typically use a modulated excitation signal for measuring impedance. In that case, the switch, S may be open when there is no signal present and may be closed whenever a signal is present. For example, if a Demodulator Signal is present for 1 ms every 100 ms, switch S would be closed during all or a part of the time that Signal In is present. Switch S may also be operated such that it does not close on every instance when Demodulator Signal is present. The switch S, may be closed on every 10thor 100thinstance when Demodulator Signal is present. A third possibility is to close switch S only when Signal Out causes the Integrator to reach an unacceptable threshold. The integrator reaching an unacceptable threshold may be indicative that the reference voltage provided by the RC combination is no longer providing a sufficiently good estimate of the nominal signal component and so needs to be updated with new information.
Turning now toFIG. 39D, there is depicted an alternative embodiment of nominal offset removal module. A further improvement on the Nominal Offset Removal module is shown inFIG. 39D. If it is desired to measure two or more different impedance signals it will be necessary to have a different nominal offset reference voltage provided to amplifier A for each signal. It is also desirable to keep the component count as low as possible. In the diagram below, S0 and S1 may be closed and S2 may be open to provide an offset reference for a first signal with the appropriate combination ofR-C1. S0 and S2 may be closed and S1 may be open to provide an offset reference for a second signal with the appropriate combination ofR-C2. This strategy allows rapid sequential measurement of two or more impedance signals.
With reference toFIG. 40, thesignal processing step370 may include general signal amplification andnoise filtering372. The step of amplification andfiltering372 may include band pass filtering to remove DC offset, for example. The respiratory waveform may then be processed to removespecific noise artifacts374 such as cardiac noise, motion noise, etc. A clean respiratory waveform may then be extracted376 along with other waveforms indicative of specific events such as obstructive sleep apnea (OSA), central sleep apnea (CSA), hypopnea, sleep stage, etc. Specific fiducial points may then be extracted and identified (e.g., type, time, and value).
The step of removingspecific noise artifacts374 may be performed in a number of different ways. However, beforesignal processing374, both cardiac and motion noise artifact may be mitigated. For example, both cardiac and motion noise artifact may be mitigated prior tosignal processing374 by selection of bio-Z vectors that are less susceptible to noise (motion and/or cardiac) as described previously. In addition, motion artifact may be mitigated beforesignal processing374 by minimizing movement of the sensing lead and electrodes relative to the body using anchoring techniques described elsewhere herein. Furthermore, motion artifact may be mitigated prior tosignal processing374 by minimizing relative movement between the current-carrying electrodes and the voltage-sensing electrodes, such as by using combined current-carrying and voltage-sensing electrodes.
After cardiac and motion artifact has been mitigated using the pre-signal processing techniques described above, both cardiac and motion artifact may be removed bysignal processing374.
For example, thesignal processing step374 may involve the use of a low pass filter (e.g., less than 1 Hz) to remove cardiac frequency noise components which typically occur at 0.5 to 2.0 Hz, whereas resting respiration frequency typically occurs below 1.0 Hz.
Alternatively, thesignal processing step374 may involve the use of a band pass or high pass filter (e.g., greater than 1 Hz) to obtain a cardiac sync signal to enable removal of the cardiac noise from the bio-Z signal in real time using an adaptive filter, for example. Adaptive filters enable removal of noise from a signal in real time, and an example of an adaptive filter is illustrated inFIG. 41. To remove cardiac artifact from the bio-Z signal which contains both cardiac noise n(k) and respiratory information s(k), a signal n′(k) that represents cardiac noise is input to the adaptive filter and the adaptive filter adjusts its coefficients to reduce the value of the difference between y(k) and d(k), removing the noise and resulting in a clean signal in e(k). Notice that in this application, the error signal actually converges to the input data signal, rather than converging to zero.
Another signal processing technique to remove cardiac noise is to combine signals from two or more bio-Z vectors wherein respiration is the predominate signal with some cardiac noise. This may also be used to reduce motion artifact and other asynchronous noise. Each of the two or more signals from different bio-Z vectors may be weighted prior to combining them into a resultant signal Vw(i). If it is assumed that (a) the respiratory bio-impedance is the largest component in each measured vector, (b) the non-respiratory signal components in one vector are substantially independent of the non-respiratory components in the other vector, and (c) the ratio of the non-respiratory component to the respiratory components in one vector is substantially equal to the same ratio in the other vector, then a simple weighting scheme may be used wherein each signal is divided by it's historic peak-to-peak magnitude and the results are added. For example, if MA=historical average peak-to-peak magnitude of signal from vector A, MB=historical average peak-to-peak magnitude of signal from vector B, VA(i)=data point (i) from vector A, VB(i)=data point (i) from vector B, then the resultant signal VW(i) (i.e., weighted average of A & B for data point (i)) may be expressed as VW(i)=VA(i)/MA+VB(i)/MB.
Yet another signal processing technique for removing cardiac noise is to subtract a first signal that is predominantly respiration from a second signal that is predominantly cardiac. For example, the first signal may be from a predominantly respiratory bio-Z vector (e.g., vector B-H) with some cardiac noise, and the second signal may be from a predominantly cardiac bio-Z vector (e.g., vector E1-E2) with some respiration signal. Each of the two signals from the different bio-Z vectors may be weighted prior to subtracting them. The appropriate weighting may be determined, for example, by calculating the power density spectra in the range of 2-4 Hz for a range of weighted differences across at least several respiratory cycles. A minimum will occur in the power density spectra for the weighted averages which are sufficiently optimal.
Motion artifact may be removed bysignal processing374 as well. Motion artifact may be identified and rejected using signal processing techniques such as monitoring voltage magnitude, testing the correlation of magnitude and phase, and/or testing correlation at two or more frequencies. Motion artifacts may cause a large change in measured bio-impedance. A typical feature of motion artifacts is that the voltage swings are much larger than respiration. Another feature is that the voltage changes are highly erratic. Using these characteristics, which will be described in more detail below, motion artifact may be removed from the respiration signal.
The step of extracting waveforms indicative of respiration andother events374 may be better explained with reference toFIGS. 42-46 which schematically illustrate various representative unfiltered bio-Z signals.FIG. 42 schematically illustrates abio-Z signal420 with representative signatures indicative normal respiration (i.e., event free) during anawake period422 and asleeping period424.FIG. 43 schematically illustrates a bio-Z signal430 with representative signatures indicative of normal respiration during sleepingperiods424 interrupted by a period of motion432 (i.e., motion artifact).FIG. 44 schematically illustrates abio-Z signal440 with representative signatures indicative of normal respiration during asleeping period424 followed by periods of hypopnea (HYP)442 andrecovery444.FIG. 45 schematically illustrates abio-Z signal450 with representative signatures indicative of normal respiration during asleeping period424 followed by periods of obstructive sleep apnea (OSA)452 and recovery454 (which typically includes an initial gasp456).FIG. 46 schematically illustrates a bio-Z signal460 with representative signatures indicative of normal respiration during asleeping period424 followed by periods of central sleep apnea (CSA)462 (which typically includes a cessation in breathing468) andrecovery464.
The step of extracting374 waveform data indicative of anawake period422 vs. asleep period424 from abio-Z signal420 may be explained in more detail with reference toFIG. 42. In addition, the step of filtering372 waveform data indicative of motion432 from a bio-Z signal430 may be explained in more detail with reference toFIG. 43. One way to determine if a person is awake or moving is to monitor the coefficient of variation (CV) of sequential peak-to-peak (PP) magnitudes over a given period of time. CV is calculated by taking the standard deviation (or a similar measure of variation) of the difference between sequential PP magnitudes and dividing it by the average (or a similar statistic) of the PP magnitudes. N is the number of respiratory cycles which occur in the selected period of time.
The CV may be calculated as follows:
CV=sd(dPP)PP_
Where:
sd(dPP)=i=1N(dPPi-dPP_)(N-1)dPP_=i=1N(dPPi)(N)dPPi=PPi+1-PPiPP_=i=1N(PPi)(N)
Generally, if the CV is greater than 0.20 over a one minute period then person is awake. Also generally, if the CV is less than 0.20 over a one-minute period then person is asleep. These events may be flagged for the step offiducial extraction378 wherein data (e.g., event duration, CV, PP range, PPmin, PPmax, etc.) may be time stamped and stored with an event identifier. If CV is greater than 1.00 over a 20 second period then body movement is affecting the bio-Z signal. By way of example, not limitation, if body movement is detected, then (a) stimulation may be delivered in an open loop fashion (e.g., based on historical respiratory data); (b) stimulation may be delivered constantly the same or lower level; or (c) stimulation may be turned off during the period of movement. The selected stimulation response to detected movement may be preset by the physician programmer or by the patient control device. Other stimulation responses may be employed as will be described hereinafter.
In each ofFIGS. 44-46, maximum and minimum peak-to-peak magnitudes (PPmax and PPmin) may be compared to distinguish hypopnea (HYP), obstructive sleep apnea (OSA), and central sleep apnea (CSA) events. Generally, PP values may be compared within a window defined by the event (HYP, OSA, CSA) and the recovery period thereafter. Also generally, the window in which PP values are taken excludes transitional events (e.g., gasp456,466). As a general alternative, peak-to-peak phases may be used instead of peak-to-peak magnitude. The hypopnea and apnea events may be flagged for the step offiducial extraction378 wherein data (e.g., event duration, CV, PP range, PPmin, PPmax, etc.) may be time stamped and stored with an event identifier.
A typical indication of hypopnea (HYP) and apnea (OSA, CSA) events is a recurrent event followed by a recovery. The period (T) of each event (where PP oscillates between PPmax and PPmin and back to PPmax) may be about 15 to 120 seconds, depending on the individual. The largest PP values observed during hypopneas and apneas are usually between 2 and 5 times larger than those observed duringregular breathing424 during sleep. The ratio of the PPmax to PPmin during recurrent hypopnea and apnea events is about 2 or more. During the event and recovery periods (excluding transitional events), PP values of adjacent respiratory cycles do not typically change abruptly and it is rare for the change in PP amplitude to be more than 50% of PPmax. One exception to this observation is that some people gasp456,466 (i.e., transitional event) as they recover from a CSA or OSA event.
The ratio of successive PP magnitudes during normal (non-event)sleep424 is mostly random. The ratio of successive PP magnitudes during apnea and hypopnea events will tend to be a non-random sequence due to the oscillatory pattern of the PP values. Recurrent apneas and hypopneas may be diagnosed by applying a statistical test to the sequence of successive PP ratios.
The step of extracting374 waveform data indicative of anhypopnea event442 from abio-Z signal440 may be explained in more detail with reference toFIG. 44. The ratio of PPmax to PPmin during recurrent hypopneas is typically between 2 and 5. This is in contrast to CSA's which have very small PPmin due to the complete cessation of breathing. This results in CSA's having PPmax to PPmin ratios larger than 5. Accordingly, hypopnea events may be detected, identified and flagged for the step offiducial extraction378 wherein data (e.g., event duration, CV, PP range, PPmin, PPmax, etc.) may be time stamped and stored with an event identifier.
The step of extracting374 waveform data indicative of anOSA event452 from abio-Z signal450 may be explained in more detail with reference toFIG. 45. Thesharp change456 in the bio-Z respiratory magnitude due to OSA is typically in the range of 1 to 4 times the magnitude of the peak-to-peak respiratory cycle magnitude. Thesharp change456 typically takes less than 5 seconds to occur. OSA tends to occur in a recurring sequence where the period (T) between sequential events is between 15 and 120 seconds. A one-minute period is commonly observed. According to these characteristics, OSA events may be detected, identified and flagged for the step offiducial extraction378 wherein data (e.g., event duration, CV, PP range, PPmin, PPmax, etc.) may be time stamped and stored with an event identifier.
The step of extracting374 waveform data indicative of a CSA event462 from a bio-Z signal460 may be explained in more detail with reference toFIG. 46. The behavior of the Bio-Z signal throughout recurrent CSA events differ from other hypopnea and OSA in three ways. First, during CSA there is complete cessation of respiratory activity which results in a flat Bio-Z signal. This means the ratio of PPmax to PPmin is typically greater than 5 during recurrent CSA events. The duration of the estimated respiratory cycle may also be used to distinguish between CSA from OSA and hypopnea. The lack of respiratory activity during CSA results in an inflated estimate for the respiratory cycle period. The PP typically does not vary by more than 50% for successive cycles. The respiratory cycle duration during a CSA event is more than twice as long as the duration of the respiratory cycles preceding the CSA event. Second, during CSA the Bio-Z magnitude will drift outside the PP magnitude range observed during respiration. It has been observed that with the onset of central sleep apnea (CSA) the magnitude and phase of the Bio-Z signal settle to a steady-state value outside the peak-to-peak range observed during the normal respiratory cycle during sleep. Third, upon arousal from CSA a person will typically gasp. This gasp results in a large PP. The PP of the first respiratory cycle following the CSA event and the PP observed during the CSA (which is essentially noise) will exceed 50% of PPmax.
With continued reference toFIG. 6, theflat portions468 of the data traces are periods of respiratory cessation. Upon arousal the subject gasps466 and the raw bio-Z signal resumes cyclic oscillation above the static impedance level observed during CSA. According to these characteristics, CSA events may be detected, identified and flagged for the step offiducial extraction378 wherein data (e.g., event duration, CV, PP range, PPmin, PPmax, etc.) may be time stamped and stored with an event identifier.
The step of extracting374 waveform data indicative of sleep stage (e.g., rapid eye movement (REM) sleep vs. no-rapid eye movement (NREM) sleep) may be performed by comparing the phase difference between a first vector and a second vector wherein the first bio-Z vector is along the lung-diaphragm-liver interface (e.g., vector A-K or vector B-K) and the second bio-Z vector is about the lung(s). Examples of the first bio-Z vector include A-K, B-K,A-E1,B-E1, and A-B. Examples of the second bio-Z vector include D-F, B-D, C-G,D-E1, andC-E1. Note that some vector combinations which share a common vector endpoint such asA-E1,D-E1 andB-E1, B-D may use a common electrode and to simplify the respiratory sensing lead or leads. Typically, during NREM sleep, the two vectors are substantially in phase. During REM sleep, the diaphragm is the primary respiratory driver and a common consequence is paradoxical motion of the ribcage and diaphragm (i.e., the two vectors are substantially out of phase). This characteristic would allow for an effective monitor of a person's ability to reach REM sleep. Accordingly, REM and NREM sleep stages may be detected, identified, and flagged for the step offiducial extraction378 wherein characteristic data (e.g., event duration, phase, etc.) may be time stamped and stored with an event identifier.
An alternative method of detecting an OSA event is to make use of a split current electrode arrangement as shown inFIG. 47 which shows the positions of three electrodes on the subject. Electrode A may be above the zyphoid, electrode B may be just above the belly button, and electrode C may be on the back a couple of inches below electrode A. Electrodes A and B are connected to a common constant current source through resistors R1 and R2. The voltage measured across the current source is a measure of the bio-impedance during normal respiration. The voltage across R1 is an indicator of the paradoxical motion associated with apnea. An unbalanced current split between R1 and R2 resulting in large bio-Z voltage swings is indicative of OSA. During normal respiration or even very deep breaths there is almost no effect on the apnea detection channel. Accordingly, OSA events may be detected, identified, and flagged for the step offiducial extraction378 wherein characteristic data (e.g., event duration, voltage swing magnitude, etc.) may be time stamped and stored with an event identifier.
Generally, the extracted378 waveform and event data may be used for therapy tracking, for stimulus titration, and/or for closed loop therapy control. For example, data indicative of apneas and hypopneas (or other events) may be stored by theINS50 and/or telemetered to the patient controlled40. The data may be subsequently transmitted or downloaded to thephysician programmer30. The data may be used to determine therapeutic efficacy (e.g., apnea hypopnea index, amount of REM sleep, etc.) and/or to titrate stimulus parameters using thephysician programmer30. The data may also be used to control stimulus in a closed loop fashion by, for example, increasing stimulus intensity during periods of increased apnea and hypopnea occurrence or decreasing stimulus intensity during periods of decreased apnea and hypopnea occurrence (which may be observed if a muscle conditioning effect is seen with chronic use). Further, the data may be used to turn stimulus on (e.g., when apnea or hypopnea events start occurring or when motion artifact is absent) or to turn stimulus off (e.g., when no apnea or hypopnea events are occurring over a present time period or when motion artifact is predominant).
Description of Stimulus Trigger Algorithms
As mentioned previously with reference toFIG. 39, the neurostimulation system described herein may operate in a closed-loop process wherein the step of deliveringstimulation390 to the targeted nerve may be a function of a sensed feedback parameter (e.g., respiration). For example, stimulation of the hypoglossal nerve may be triggered to occur during the inspiratory phase of respiration. In a health human subject, the hypoglossal nerve is triggered about 300 mS before inspiration. Accordingly, a predictive algorithm may be used to predict the inspiratory phase and deliver stimulation accordingly.FIG. 48 schematically illustrates asystem480 including devices, data and processes for implementing a self-adjusting predictive trigger algorithm.
The system components482 involved in implementing the algorithm may include the physician programmer (or patient controller), INS and associated device memory, and the respiratory sensor(s). The sensors and device memory are the sources of real-time data and historical fiducial data which the current algorithm uses to generate a stimulation trigger signal. The data484 utilized in implementing the algorithm may include patient specific data derived from a sleep study (i.e., PSG data), data from titrating the system post implantation, and historic and real-time respiratory data including respiratory and event fiducials. Theprocesses486 utilized in implementing the algorithm may include providing a default algorithm pre-programmed in the INS, patient controller or physician programmer, modifying the default algorithm, and deriving a current algorithm used to generate a trigger signal488.
More specifically, theprocesses486 utilized in implementing a predictive trigger algorithm may involve several substeps. First, a default algorithm may be provided to predict onset of inspiration from fiducial data. Selecting an appropriate default algorithm may depend on identifying the simplest and most robust fiducial data subsets which allow effective prediction of onset. It also may depend on a reliable means of modifying the algorithm for optimal performance. Second, modification of the default algorithm may require a reference datum. The reference datum may be the estimated onset for past respiratory cycles. It is therefore useful to precisely estimate inspiratory onset for previous respiratory cycles from historical fiducial data. This estimation of inspiratory onset for previous respiratory cycles may be specific to person, sensor location, sleep stage, sleep position, or a variety of other factors. Third, the current algorithm may be derived from real-time and historical data to yield a stimulation trigger signal488.
As alluded to above, a trigger algorithm, such as, for example,trigger algorithm4700 depicted inFIG. 47A, may be applied to a detected respiratory signal to begin and/or control delivery of the stimulation signal. As illustrated,trigger algorithm4700 may include a plurality of sub-routines4701-4703 for performing various analyses on a sensed respiratory signal. These sub-routines may include, but are not limited to, performingpeak detection4701, error checking4702, andprediction4703, on a detected respiratory signal.
With reference now toFIG. 47D, there is depicted an exemplary sensedrespiratory signal4750.Respiratory signal4750 may be displayed as a substantially sinusoidal waveform having a component that varies with time. As shown inFIG. 47D,respiratory signal4750 may include a plurality of peaks, such as, for example, the peak located at v4t4, and a plurality of valleys, such as, for example, the valley located v−4t−4. Therefore, as will be discussed in greater detail below,peak detection sub-routine4701 may be applied to sensedrespiratory signal4750 to detect the peaks ofsignal4750.Error checking sub-routine4702 may be applied to signal4750 to, among other things, ensuresignal4750 is an accurate representation of a patient's respiration and free from undesirable artifacts caused by, for example, a patient's movement or cardiac activity.Prediction sub-routine4703 may then be applied to signal4750 to predict when future peaks will occur in accordance with the sensedsignal4750.
With reference toFIG. 47B,peak detection4701 may include a plurality of steps4701a-g. Step4701a may include first detecting the peaks, such as, for example, the peak located at v4t4, ofsignal4750. The detected peaks may be an indication of when onset of expiration occurs during the monitored respiratory cycles. Next, step4701b may include acquiring and/or considering a new voltage Vk, where Vkmay be the most recently acquired data point time Tkunder consideration, where a number of recently acquired data points may be under consideration.Step4701c may determine whether the data points under consideration meet the criteria to indicate that a minimum (min) peak has been detected. One example of such a criteria to indicate a minimum peak has been detected is if the oldest data point under consideration, Vk+mis less than more recent data points under consideration, (Vk+m−1. . . Vk), which can be expressed mathematically as Vk+m≤min (Vk+m−1. . . Vk). Another example of such a criteria to indicate a minimum peak has been detected is if the most recent data point under consideration, Vk, is greater than all other less-recently acquired data points under consideration, (Vk+m. . . Vk+1), which can be expressed mathematically as Vk≥max (Vk+m. . . Vk+1). If the criteria for detecting a minimum peak is not met, step4701b may be repeated to acquire and/or consider a new voltage Vk. If the criteria has been met,step4701d may declare a minimum peak reference. Next, step4701e may again acquire and/or consider a new voltage Vk. Subsequently, step4701f may determine whether the data points under consideration meet the criteria to indicate a maximum peak has been detected. One example of such a criteria to indicate a maximum peak has been detected is if the oldest data point under consideration, Vk+m, is greater than more recent data points under consideration (Vk+m−1. . . Vk), which can be expressed mathematically as Vk+m≥max (Vk+m−1. . . Vk). Another example of such a criteria to indicate a maximum peak has been detected is if the most recent data point under consideration, Vk, is less than all other less-recently acquired data points under consideration, (Vk+m. . . Vk+1), which can be expressed mathematically as Vk≥max (Vk+m. . . Vk+1). If the criteria for detecting a maximum peak is not met, step4701e may be repeated to acquire and/or consider a new voltage Vk. If the criteria has been met, step4701g may declare a maximum peak, andtrigger algorithm4700 may proceed to error-checking sub-routine4702. The declared peak will depend on the criteria used for peak detection. For example, if the criteria for detecting a peak was based on comparing Vkto less recently acquired data points, (Vk+m. . . Vk+1), then the peak magnitude and time would be declared to be Vk+m/2, tk+m/2. As another example, if the criteria for detecting a peak was based on comparing the oldest considered data point, Vk+m, to more recently acquired data points (Vk+m−1. . . Vk), then the peak magnitude and time would be declared to be Vk+m, tk+m.
With reference now toFIG. 47C, error-checking sub-routine4702 may include a plurality of steps4702a-e to determine whether a sensed respiratory signal may be adequate for respiration detection. For example, step4702a, peak correction, may include receiving information relating to the peaks detected instep4701 and corrections, as necessary. Next, steps4702b-e may include analyzing the sensed respiratory signal to determine whether the signal includes “noise” caused by a patient's movement (4702b), whether the signal is sub-threshold (e.g., has a relatively low amplitude) (4702c), whether the signal is sufficiently stable (4702d), and whether the inversion detection is possible with the sensed signal (4702e). If the sensed signal passes all of error-checking steps4702b-e,trigger algorithm4700 may proceed toprediction sub-routine4703. However, if the sensed signal fails any of steps4702b-e, the trigger algorithm may terminate and the pulse generator (e.g., INS50) may either cease stimulation, continue stimulation with continuous pulses of predetermined duration, and/or continue to stimulate at the same or a fraction (e.g., one quarter) of the stimulation rate for the most recently measured respiratory cycle, as discussed in greater detail below.
As described above, a peak is declared for a given set of data points under consideration when a peak detection criteria is met. The declared peak itself may be used in further algorithm calculations or a more precise estimate of peak time and voltage may be calculated. The more precise estimates of peak time and voltage are referred to as the peak correction. With regard to step4702a, peak correction may be calculated as follows:
ΔVpk,i=Vpk,j−Vpk,i−1for −n≤i≤n
Vpk,0is defined to be the declared peak for which a correction is being calculated. The difference in voltage between successive data points is calculated for a given number of data points, n, to either side of the declared peak.
ΔVpk,0th=12nΣ(ΔVpk,i)
The peak in signal ideally occurs when the rate of change of the signal is zero. Taking successive differences in measured voltage is an approximation to the rate of change of the signal. Linear regression is used on a range of successive differences to estimate the point in time when the rate of change is zero. Due to the fact that the data points are collected at equal increments of time, calculating the statistics ΔVpk,0th, ΔVpk,1stand DEN allows a simple calculation based on linear regression to estimate the point in time at which the rate of change of the signal is zero.
ΔVpk,1st=Σ(i*ΔVpk,i)for-ni<nDEN=Σ(i2)for-ninCorrection=ΔVpk,0th(DENΔVpk,1st)
Additionally, an estimated peak time after correction may be determined as follows:
t′pk,0=tpk,0+Correction
With regards to step4702e, a peak curvature estimate for inversion detection can be obtained from one of the statistics, ΔVpk,1st, calculated for peak correction. Maximum peaks are sharper than minimum peaks and so typically have higher values of ΔVpk,1st. One means of determining if a signal is inverted would be to compare the values of ΔVpk,1stfor a series of maximum peaks to a series of minimum peaks.
With renewed reference toFIG. 47A,prediction sub-routine4703 may include predicting the time between sequentially identified peaks with either a parametric option or a non-parametric option. The parametric option makes a prediction of the duration of the next respiratory period based on the average duration of recent respiratory cycles and the rate of change of the duration of recent respiratory cycles. The parametric option also takes advantage of the fact that data points are collected at equal increments of time which simplifies the linear regression calculation. The parametric option may be defined as follows:
Δti=ti−ti−1
Zeroth order estimate of next peak.
Δt0,0th=1/h·Σ(Δti),for1in
where n is the number of past respiration cycles used
First Order Estimate
Δt0,1st=Σ(i-(n+12)*Δti),for1inDEN1=Σ((i-(n+12))2),for1in
Predicted Interval Length for Current Respiration Cycle
Δt0,pred=Δt0,0th+(Δt0,1stDEN1)·(n+12)
Next Predicted Offset at
t0,pred=ti+Δt0,pred
Begin therapy delivery at:
ttherapy=t1+(1−DC)*Δt0,pred, where DC may be the allowable duty cycle for therapy delivery.
The non-parametric option is very similar to the parametric option in that it also estimates the duration of the next respiratory period based on the nominal duration of recent respiratory cycles and the rate of change of the duration of recent respiratory periods. The method is explained in more detail in “Nonparametric Statistic Method” by Hollander and Wolfe in sections related to the Theil statistic and the Hodges-Lehman, there disclose of which is incorporated herein by reference. The non-parametric prediction method may be defined as follows:
Δti=ti−ti−1
Zeroth Order Estimate
Δt0,oth=½ median{Δti+Δtj, i+∈0≤j≤1, . . . , n}
Where ∈0is optimally 0, 1, 2 or 3
First Order Estimate
Sij=Δtj-Δtij-i1i+1<jn
where ∈1is optimally 0, 1, 2, or 3
Δt0,1st=median{Sij, 1≤i≤∈1<j≤n}
Predicted Interval Length for Current Respiration cycle
Δt0,pred=Δt0,0th+Δt0,1st·(n+12)
Next Predicted Offset
t0,pred=t1+Δt0,pred
Begin Therapy Delivery at
ttherapy=t1+(1−DC))*Δt0,pred, where DC may be the allowable duty cycle for therapy delivery.
Stimulation may then commence at the calculated ttherapy.
With reference toFIG. 48, a self adjusting predictive algorithm may be implemented in the following manner.
The Programmer block illustrates means by which PSG-derived data may be uploaded into the device.
The Sensors and Device Memory block includes the sources of real-time data and historical fiducial variables which the current algorithm uses to generate a stimulation trigger signal.
The Patient PSG Titration Data block includes conventional polysomnographic (PSG) data obtained in a sleep study. A self-adjusting predictive algorithm utilizes a reference datum to which the algorithm can be adjusted: Onset may be defined as onset of inspiration as measured by airflow or pressure sensor used in a sleep study, for example. Estimated Onset may be defined as an estimate of Onset calculated solely from information available from the device sensors and memory. To enable the predictive algorithm to be self-adjusting, either Onset or Estimated Onset data is used. During actual use, the implanted device will typically not have access to Onset as that would require output from an airflow sensor. The device then may rely on an estimate of Onset or Estimated Onset. The calibration of Estimated Onset to Onset may be based on PSG data collected during a sleep study. The calibration may be unique to a person and/or sleep stage and/or sleep position and/or respiratory pattern.
The Historical Fiducial Variables block represents the Historical Fiducial Variables (or data) which have been extracted from the bio-Z waveform and stored in the device memory. This block assumes that the raw sensor data has been processed and is either clean or has been flagged for cardiac, movement, apnea or other artifacts. Note that fiducial data includes fiducials, mathematical combinations of fiducials or a function of one or more fiducials such as a fuzzy logic decision matrix.
The Real-Time Data and Historical Fiducial Variables block incorporates all the information content of the Historical Fiducial Variables block and also includes real-time bio-Z data.
The Default Algorithm block represents one or more preset trigger algorithms pre-programmed into the INS or physician programmer. The default algorithm used at a specific point in time while delivering therapy may be selected from a library of pre-set algorithms. The selection of the algorithm can be made automatically by the INS based on: patient sleep position (position sensor), heart rate (detectable through the impedance measuring system) or respiration rate. Clinical evidence supports that the algorithm used to predict the onset of inspiration may be dependant on sleep position, sleep state or other detectable conditions of the patient.
The Modify Algorithm block represents the process of modifying the Default Algorithm based on historical data to yield the Current Algorithm. Once the calibration of Estimated Onset to Onset is resident in the device memory it can be used to calculate Estimated Onset for past respiratory cycles from Fiducial Variables. The variable used to represent the Estimated Onset will be TEST or TEST(i) where the “i” indicates the cycle number. Note that Estimated Onset is calculated for past respiratory cycles. This means that sensor fiducial variables which either proceed or follow each Onset event may be used to calculate the Estimated Onset.
The Current Algorithm block represents the process of using the Modified Default Algorithm to predict the next inspiratory onset (Predicted Onset). The Predicted Onset for the next respiratory cycle may be calculated from real-time data and historical fiducial variables. The calculation may be based on the Modified Default Algorithm. Modification of the Modified Default Algorithm to derive the Current Algorithm may be dependent on the calibration of Estimated Onset to Onset which was input from the physician programmer and may be based on comparison of real-time bio-Z data to data collected during a PSG titration study. The Current Algorithm may use historic and/or real-time sensor fiducial variables to predict the next onset of inspiration. This predicted onset of inspiration may be referred to as Predicted Onset. The variable used to represent Predicted Onset may be TPRED or TPRED(i) where the “i” indicates the respiratory cycle.
The Stimulation Trigger Signal block represents the Current Algorithm generating a trigger signal which the device uses to trigger stimulation to the hypoglossal nerve.
FIG. 49 is a table of some (not all) examples of waveform fiducials which can be extracted from each respiratory cycle waveform. For each fiducial there is a magnitude value and a time of occurrence. Each waveform has a set of fiducials associated with it. As a result, fiducials may be stored in the device memory for any reasonable number of past respiratory cycles. The values from past respiratory cycles which are stored in device memory are referred to as Historical Fiducial Variables.
The graphs illustrated inFIG. 50 are examples of fiducials marked on bio-Z waveforms. The first of the three graphs illustrate the bio-impedance signal after it has been filtered and cleared of cardiac and motion artifacts. The first graph will be referred to as the primary signal. The second graph is the first derivative of the primary signal and the third graph is the second derivative of the primary signal. Each graph also displays a square wave signal which is derived from airflow pressure. The square wave is low during inspiration. The falling edge of the square wave is onset of inspiration.
Due to the fact that it may be difficult to identify onset of inspiration in real-time from respiratory bio-impedance, a goal is to construct an algorithm which can reliably predict onset of inspiration “T” for the next respiratory cycle from information available from the current and/or previous cycles. A reliable, distinct and known reference point occurring prior to onset of inspiration, “T”, is “A”, the peak of the primary signal in the current cycle. As can be seen inFIG. 50, the upper peak of the bio-Z waveform “A” approximately corresponds to the onset of expiration “O.” A dependent variable tT−PKis created to represent the period of time between the positive peak of the primary signal for the current cycle, t·Vmax(n), indicated by “An” on the graph, and onset of inspiration for the next cycle, t·onset(n+1), indicated by “T” on the graph. The variable tT−PKmay be defined as:
tT−PK=t·onset(n+1)−t·Vmax(n)
Note that t·Vmax could be replaced by any other suitable fiducial in defining a dependent variable for predicting onset.
A general model for a predictive algorithm may be of the following form:
tT−PK=f(fiducials extracted from current and/or previous cycles)
A less general model would be to use a function which is a linear combination of Fiducial Variables and Real-Time Data.
The following fiducials may be both highly statistically significant and practically significant in estimating T:
t·Vmax(n)=the time where positive peak occurs for the current cycle;
t·dV·in(n)≈the time of most positive 1stderivative during inspiration for the current cycle; and
t·Vmax(n−1)=the time of positive peak for the previous cycle.
This model can be further simplified by combining the variables as follows:
Δt·pk(n)=t·Vmax(n)−t·Vmax(n−1)
Δt·in(n)=t·Vmax(n)−t·dV·in(n)
Either Δt·pk(n) or Δt·in(n) is a good predictor of Onset.
The following example uses Δt·pk(n). The time from a positive peak until the next inspiration onset can be estimated by:
Tpred=t·Vmax(n)+k0+k1*Δt·pk(n)
The coefficients k0 and k1 would be constantly modified by optimizing the following equation for recent historical respiratory cycles against Test:
Test≈t·Vmax(n)+k0+k1*Δt·pk(n)
Thus, the predictive trigger time Tpredmay be determined by adding tT−PKto the time of the most recent peak (PK) of the bio-Z signal, where:
tT−PK=k0+k1*Δt·pk(n)
The predictive equation we are proposing is based on the fact that the very most recent cycle times should be negatively weighted. Regression analysis supports this approach and indicates a negative weighting is appropriate for accurate prediction of onset. Thus, predicting onset is more effective if the most recent historical cycle time is incorporated into an algorithm with a negative coefficient.
As noted above, stimulation may be delivered for only a portion of the respiratory cycle, such as, for example, during inspiration. Additionally, it may be desirable to begin stimulation approximately 300 milliseconds before the onset of inspiration to more closely mimic normal activation of upper airway dilator muscles. However, predicting and/or measuring inspiration, in particular, the onset of inspiration, may be relatively challenging. Thus, since the onset of expiration may be relatively easy to measure and/or predict (as discussed in greater detail below) when an adequate measure of respiration is available, it is contemplated that stimulation may be triggered as a function of expiration onset.
Turning now toFIG. 50A, there is depicted an exemplaryrespiratory waveform5500 for two complete respiratory cycles A and B. In analyzingexemplary waveform5500, it may be determined that peaks M of thewaveform5500 may indicate onset of the expiratory phases of respiration cycles A and B. Furthermore, it may be discovered that peaks M occur at regular intervals of approximately 3-4 seconds. Thus, it may be relatively easy to predict the occurrence of subsequent peaks M, and consequently, the onset of expiration for future respiratory cycles.
Therefore, in order to deliver a stimulus to a patient in accordance with the principles of the present disclosure, the start of stimulation may be calculated by first predicting the time intervals between the start of expiration for subsequently occurring respiratory cycles. Next, in order to capture the entire inspiratory phase, including the brief pre-inspiratory phase of approximately 300 milliseconds, stimulation may be started at the time N that is prior to the next onset of expiration by approximately 30% to 50% of the time between subsequently occurring expiratory phases. Stimulating less than 30% or more than 50% prior to the next expiratory phase may result in an inadequate stimulation period and muscle fatigue, respectively.
In some embodiments, however, it is contemplated that an adequate measure of respiration may not be available, such as, for example, when a relied upon signal has failed. In these embodiments, it is contemplated that the implanted neurostimulator system may be configured to respond in one or more of the following three ways. First, the implanted neurostimulator may completely cease stimulation until an adequate signal is acquired. Second, the neurostimulator may deliver continuous simulation pulses of predetermined durations (e.g., up to 60 seconds) until an adequate signal is acquired; or if an adequate signal is not acquired in this time, the stimulation will be turned off. Third, the neurostimulator may continue to stimulate at the same or a fraction (e.g., one quarter) of the stimulation rate for the most recently measured respiratory cycle. That is to say, the neurostimulator may deliver stimulation pulses of relatively long durations at a frequency that is less than the frequency of stimulation utilized with an adequate measure of respiration. Alternatively, the neurostimulator may deliver stimulation pulses of relatively short durations at a frequency that is greater than the frequency used with an adequate measure of respiration.
Description of an Exemplary Stimulation Pulse
Turning now toFIG. 50B, there is depicted an exemplary stimulation pulse waveform5000 that may be emitted from an INS in accordance with the principles of the present disclosure. Typically, exemplary stimulation pulse waveform5000 may include a square wave pulse train having one or moresquare wave pulses5001 of approximately 1 to 3 volts in amplitude, a duration of approximately 100 ms, and a frequency of approximately 30 Hz, assuming a 1000 ohm impedance at the electrodes and a constant current or voltage.
In some embodiments, exemplary stimulation pulse waveform5000 may include a bi-phasic charge balanced waveformsquare pulses5001 and5002, as depicted inFIG. 50B.Square pulse5002 may be included in waveform5000 to, among other things, promote efficient stimulation and/or mitigate electrode corrosion. However,square pulse5002 may be excluded from waveform5000 as desired. Furthermore, although the depicted exemplary waveform5000 includessquare pulse5002 that exactly balances thestimulation wave pulse5001, in certain circumstances,square pulse5002 may not exactly balance thestimulation wave pulse5001, and may not be a square pulse.
In some embodiments, exemplary stimulation pulse waveform5000 may include the delivery of a low amplitude (e.g., below the stimulation threshold), long duration, pre-stimulation pulse5004. The pre-stimulation pulse5004 may include any suitable low amplitude, long duration pulse, and may be provided approximately 0.5 ms before the delivery of afirst stimulation pulse5001.
Pre-stimulation pulse5004 may facilitate selectively stimulating certain fibers of a nerve, such as, for example, the hypoglossal nerve or the superior laryngeal nerve. In particular, when stimulating the hypoglossal nerve, the presence of a pre-stimulation pulse, such as, for example, pulse5004, before a stimulation pulse (e.g., thebi-phasic stimulation pulse5001 depicted inFIG. 50B) may serve to saturate the large diameter fibers of the nerve so as to allow thestimulation pulse5001 to only affect (e.g., stimulate) the smaller diameter fibers of the nerve. In circumstances where a nerve (e.g., the hypoglossal nerve) may be stimulated for extended periods of time, a pre-stimulation pulse5004 may be selectively introduced to waveform5000, so as to permit selective switching between stimulating the large and small diameter fibers of the nerve, in order to reduce muscle fatigue. Similarly, in situations where OSA may be treated by stimulating the superior laryngeal nerve to open the upper airway through a reflex mechanism, the presence of pre-stimulation pulse5004 may serve to saturate the larger diameter efferent fibers so as to allow thestimulation pulse5001 to only affect the smaller diameter afferent fibers of the nerve.
Description of External (Partially Implanted) System
With reference toFIGS. 51A and 51B, an example of an external neurostimulator system inductively coupled to an internal/implanted receiver is shown schematically. The system includes internal/implanted components comprising areceiver coil910, a stimulator lead60 (includinglead body62, proximal connector and distal nerve electrode64). Any of the stimulation lead designs and external sensor designs described in more detail herein may be employed in this generically illustrated system, with modifications to position, orientation, arrangement, integration, etc. made as dictated by the particular embodiment employed. The system also includes external components comprising a transmit coil912 (inductively linked toreceiver coil910 when in use), an external neurostimulator or external pulse generator920 (ENS or EPG), and one or more externalrespiratory sensors916/918.
As illustrated, thereceiver coil910 is implanted in a subcutaneous pocket in the pectoral region and thestimulation lead body62 is tunneled subcutaneously along the platysma in the neck region. Thenerve electrode64 is attached to the hypoglossal nerve in the submandibular region.
Thetransmitter coil912 may be held in close proximity to thereceiver coil910 by any suitable means such as an adhesive patch, a belt or strap, or an article of clothing (e.g., shirt, vest, brazier, etc.) donned by the patient. For purposes of illustration, thetransmitter coil912 is shown carried by a t-shirt915, which also serves to carry theENS920 and respiratory sensor(s)916,918. TheENS920 may be positioned adjacent the waist or abdomen away from the ribs to avoid discomfort while sleeping. The respiratory sensor(s)916,918 may be positioned as a function of the parameter being measured, and in this embodiment, the sensors are positioned to measure abdominal and thoracic/chest expansion which are indicative of respiratory effort, a surrogate measure for respiration. The external components may be interconnected bycables914 carried by the shirt or by wireless means. The shirt may incorporate recloseable pockets for the external components and the components may be disconnected from the cables such that the reusable components may be removed from the garment which may be disposed or washed.
The transmittingcoil antenna912 and the receivingcoil antenna910 may comprise air core wire coils with matched wind diameters, number of wire turns and wire gauge. The wire coils may be disposed in a disc-shaped hermetic enclosure comprising a material that does not attenuate the inductive link, such as a polymeric or ceramic material. The transmittingcoil912 and the receivingcoil910 may be arranged in a co-axial and parallel fashion for coupling efficiency, but are shown side-by-side for sake of illustration only.
Because power is supplied to the internal components via an inductive link, the internal components may be chronically implanted without the need for replacement of an implanted battery, which would otherwise require re-operation. Examples of inductively powered implantable stimulators are described in U.S. Pat. No. 6,609,031 to Law et al., U.S. Pat. No. 4,612,934 to Borkan, and U.S. Pat. No. 3,893,463 to Williams, the entire disclosures of which are incorporated herein by reference.
With reference toFIGS. 51C-51G, alternative embodiments of an external neurostimulator system inductively coupled to an internal/implanted receiver are schematically shown. These embodiments are similar to the external embodiment described above, with a few exceptions. In these embodiments, thereceiver coil910 is implanted in a positioned proximate the implantedstimulation lead body62 andnerve electrode64. Thereceiver coil910 may be positioned in a subcutaneous pocket on the platysma muscle under the mandible, with thelead body62 tunneling a short distance to thenerve electrode64 attached to the hypoglossal nerve. Also in these embodiments, the respiratory sensor(s)916/918 may be integrated into theENS920 and attached to a conventionalrespiratory belt922 to measure respiratory effort about the abdomen and/or chest. Anexternal cable914 connects theENS920 to thetransmitter coil912.
In the embodiment ofFIG. 51D, thetransmitter coil912 is carried by anadhesive patch924 that may be placed on the skin adjacent thereceiver coil910 under the mandible. In the embodiment ofFIG. 51E, thetransmitter coil912 is carried by an under-chin strap926 worn by the patient to maintain the position of thetransmitter coil912 adjacent thereceiver coil910 under the mandible. In the embodiment ofFIG. 51F, thereceiver coil910 may be positioned in a subcutaneous pocket on the platysma muscle in the neck, with the lead body122 tunneling a slightly greater distance. Thetransmitter coil912 may be carried by aneck strap928 worn by the patient to maintain the position of thetransmitter coil912 adjacent thereceiver coil910 in the neck.
With reference toFIGS. 51G-51K, additional alternative embodiments of an external neurostimulator system inductively coupled to an internal/implanted receiver are schematically shown. These embodiments are similar to the external embodiment described above, with a few exceptions. As above, thereceiver coil910 may be positioned in a subcutaneous pocket on the platysma muscle under the mandible, with thelead body62 tunneling a short distance to thenerve electrode64 attached to the hypoglossal nerve. However, in these embodiments, the ENS920 (not shown) may be located remote from the patient such as on the night stand or headboard adjacent the bed. TheENS920 may be connected via acable930 to alarge transmitter coil912 that is inductively coupled to thereceiver coil910. Therespiratory sensor916 may comprise a conventionalrespiratory belt922 sensor to measure respiratory effort about the abdomen and/or chest, and sensor signals may be wirelessly transmitted to theremote ENS920. As compared to other embodiments described above, thetransmitter coil912 is not carried by the patient, but rather resides in a proximate carrier such as a bed pillow, under a mattress, on a headboard, or in a neck pillow, for example. Because thetransmitter coil912 is not as proximate the receiver coil as in the embodiments described above, the transmitter coil may be driven by a high powered oscillator capable of generating large electromagnetic fields.
As shown inFIG. 51H, thetransmitter coil912 may be disposed in abed pillow934. As shown inFIG. 51I, thetransmitter coil912 may comprise a series of overlapping coils disposed in abed pillow934 that are simultaneously driven or selectively driven to maximize energy transfer efficiency as a function of changes in body position of the patient corresponding to changes in position of thereceiver coil910. This overlapping transmitter coil arrangement may also be applied to other embodiments such as those described previously wherein the transmitter coil is carried by an article donned by the patient. InFIG. 51J, two or more transmitter coils912 are carried by orthogonal plates936 arranged as shown to create orthogonal electromagnetic fields, thereby increasing energy transfer efficiency to compensate for movement of the patient corresponding to changes in position of thereceiver coil910.FIG. 51J also illustrates a non-contactrespiratory sensor916 arrangement as utilized for detecting sudden infant death syndrome (SIDS). As shown inFIG. 51K, two orthogonal transmitter coils912 are located on each side of aneck pillow938, which is particularly beneficial for bilateral stimulation wherein areceiver coil910 may be located on either side of the neck.
With reference toFIGS. 51L (front view) and51M (rear view), externalrespiratory effort sensors916/918 are schematically shown incorporated into astretchable garment945 donned by the patient. Thesensors916/918 generally include one or more inductive transducers and an electronics module942. The inductive transducers may comprise one or more shaped (e.g., zig-zag or sinusoidal) stranded wires to accommodate stretching and may be carried by (e.g., sewn into) thegarment945 to extend around the patient's abdomen and chest, for example. As the patient breathes, the patient's chest and/or abdomen expands and contracts, thus changing the cross-sectional area of the shape (i.e., hoop) formed by the wire resulting in changes in inductance. The electronics module may include an oscillator (LC) circuit with the inductive transducer (L) comprising a part of the circuit. Changes in frequency of the oscillator correspond to changes in inductance of the shaped wires which correlate to respiratory effort. The electronics module may be integrated with an ENS (not shown) or connected to an ENS via a wired or wireless link for triggering stimulus as described previously.
Thegarment945 may include features to minimize movement artifact and accommodate various body shapes. For example, thegarment945 may be form-fitting and may be sleeveless (e.g., vest) to reduce sensor artifacts due to arm movement. Further, thegarment945 may be tailored to fit over the patient's hips with a bottom elastic band which helps pull the garment down and keep thesensors916/918 in the proper location.
Description of a Specific External (Partially Implanted) Embodiment
With reference toFIGS. 52A-52G a specific embodiment utilizing an external neurostimulator system inductively coupled to an internal/implanted receiver is schematically shown. With initial reference toFIG. 52A, the illustrated hypoglossal nerve stimulator includes several major components, namely: an implantable electronics unit that derives power from an external power source; a stimulation delivery lead that is anchored to the nerve or adjacent to the nerve and provides electrical connection between the electronics unit and the nerve, an external (non-implanted) power transmitting device that is inductively coupled with the implant to convey a powering signal and control signals; a power source for the external device that is either small and integrated into the body-worn coil and transmitter or is wired to the transmitter and transmit induction coil and can be powered by primary or secondary batteries or can be line powered; and a respiratory sensor such as those described previously.
These components may be configured to provide immediate or delayed activation of respiration controlled stimulation. Initiation of the stimulation regimen may be by means of activation of an input switch. Visual confirmation can be by an LED that shows adequate signal coupling and that the system is operating and is or will be applying stimulation. As a means of controlling gentleness of stimulation onset and removal, either pulse width ramping of a constant amplitude stimulation signal can be commanded or amplitude of a constant pulse width stimulation signal or a combination thereof can be performed.
The electrical stimulation signal is delivered by the stimulation lead that is connected to the implanted nerve stimulator and attached to or in proximity of a nerve. The implanted electronics unit receives power through a magnetically coupled inductive link. The operating carrier frequency may be high enough to ensure that several cycles (at least 10) of the carrier, comprise the output pulse. The operating frequency may be in a band of frequencies approved by governmental agencies for use with medical instruments operating at high transmitted radio frequency (RF) power (at least 100 milliwatts). For example, the operating frequency may be 1.8 MHz, but 13.56 MHz is also a good candidate since it is in the ISM (Industrial/Scientific/Medical) band. The non-implanted (external) transmitter device integrates respiration interface, waveform generation logic and transmit power driver to drive an induction coil. The power driver generates an oscillating signal that drives the transmitter induction coil and is designed to directly drive a coil of coil reactance that is high enough or can be resonated in combination with a capacitor. Power can come from a high internal voltage that is used to directly drive the transmit induction coil or power can come from a low voltage source applied to a tap point on the induction coil.
With reference toFIGS. 52B-52E, the waveform generation logic may be used to modulate the carrier in such a way that narrow gaps in the carrier correspond to narrow stimulation pulses. When stimulator pulses are not needed, interruptions to the carrier are stopped but the carrier is maintained to ensure that power is immediately available within the stimulator upon demand. Presence or absence of electrical nerve stimulation is based on respiration or surrogates thereof. The transmitted signal may comprise a carrier of about 1.8 MHz. To control the implanted electronics unit to generate individual nerve stimulation pulses, the carrier signal is interrupted. The duration of the interruption is about equal to the duration of the output stimulation pulse. The stimulation pulses may be about 110 microseconds in duration and are repeated at a rate of approximately 33 per second. In addition, multiple pulses can be transmitted to logic within the implant to control stimulation pulse amplitude, pulse width, polarity, frequency and structure if needed. Further, onset and removal of stimulation can be graded to manage patient discomfort from abruptness. Grading may comprise pulse width control, signal amplitude control or a combination thereof.
An indicator (not shown) may be used to show when the transmitter is properly positioned over the implant. The indicator may be a part of the transmitter or by way of communication with the transmitter, or a part of related patient viewable equipment. Determination of proper position may be accomplished by monitoring the transmitter power output loading relative to the unloaded power level. Alternatively, the implant receive signal level transmitted back by a transmitter within the implant may be monitored to determine proper positioning. Or, the implant receive signal level that is communicated back to the transmitter by momentarily changing the loading properties presented to the transmitter, such a shorting out the receive coil may be monitored to determine proper positioning. Such communication may be by means of modulation such as pulse presence, pulse width, pulse-to-pulse interval, multi-pulse coding.
The transmitter may be powered by an internal primary power source that is used until it is exhausted, a rechargeable power source or a power source wired to a base unit. In the case of the wired base unit, power can be supplied by any combination of battery or line power.
The respiration interface may transduce sensed respiratory activity to an on-off control signal for the transmitter. Onset of stimulation may be approximately correlated slightly in advance of inspiration and lasts through the end of inspiration, or onset may be based on anticipation of the next respiration cycle from the prior respiration cycle or cycles. The respiration sensor may comprise any one or combination of devices capable of detecting inspiration. The following are examples: one or more chest straps; an impedance sensor; an electromyographical measurement of the muscles involved with respiration; a microphone that is worn or is in proximity to the patients' face; a flow sensor; a pressure sensor in combination with a mask to measure flow; and a temperature sensor to detect the difference between cool inspired air versus warmed expired air.
The circuit illustrated inFIG. 52F may be used for the implanted electronics unit. There are five main subsystems within the design: a receive coil, a power rectifier, a signal rectifier, an output switch and an output regulator. The signal from the inductive link is received by L1 which is resonated in combination with C1 and is delivered to both the power and signal rectifiers. Good coupling consistent with low transmitter coil drive occurs when the transmit coil diameter is equal to the receive coil diameter. When coil sizes are matched, coupling degrades quickly when the coil separation is about one coil diameter. A large transmit coil diameter will reduce the criticality of small coil spacing and coil-to-coil coaxial alignment for maximum signal transfer at the cost of requiring more input drive power.
The power rectifier may comprise a voltage doubler design to take maximum advantage of lower signal levels when the transmit to receive coil spacing is large. The voltage doubler operates with an input AC voltage that swing negative (below ground potential) causes D1 to conduct and forces C2 to the maximum negative peak potential (minus a diode drop). As the input AC voltage swings away from maximum negative, the node of C2, D1, D2 moves from a diode drop below ground to a diode drop above ground, forward biasing diode D2. Further upswing of the input AC voltage causes charge accumulated on C2 to be transferred through D2 to C3 and to “pump up” the voltage on C3 on successive AC voltage cycles. To limit the voltage developed across C3 so that an over-voltage condition will not cause damage, and Zener diode, D3 shunts C3. Voltage limiting imposed by D3 also limits the output of the signal rectifier section. The power rectifier has a long time constant, compared to the signal rectifier section, of about 10 milliseconds.
The signal rectifier section may be similar in topology to the power rectifier except that time constants are much shorter—on the order of 10 microseconds—to respond with good fidelity to drop-outs in the transmitted signal. There is an output load of 100K (R1) that imposes a controlled discharge time constant. Output of the signal rectifier is used to switch Q1, in the output switching section, on and off.
The output switching section compares the potential of C3 to that across C5 by means of the Q1, Q2 combination. When there is a gap in the transmitted signal, the voltage across C5 falls very rapidly in comparison with C3. When the voltage difference between C5 and C3 is about 1.4 volts, Q1 and Q2 turn on. Q1 and Q2 in combination form a high gain amplifier stage that provides for rapid output switching time. R3 is intended to limit the drive current supplied to Q2, and R2 aids in discharging the base of Q2 to improve the turn-off time.
In the output regulator section, the available power rectifier voltage is usually limited by Zener diode D3. When the coil separation becomes suboptimal or too large the power rectifier output voltage will be come variable as will the switched voltage available at the collector of Q2. For proper nerve stimulation, it may be necessary to regulate the (either) high or variable available voltage to an appropriate level. An acceptable level is about 3 volts peak. A switched voltage is applied to Zener diode D6 through emitter follower Q3 and bias resistor R5. When the switched voltage rises to a level where D6 conducts and develops about 0.6 volts across R4 and the base-emitter junction of Q4, Q4 conducts. o Increased conduction of Q4 is used to remove bias from Q3 through negative feedback. Since the level of conduction of Q4 is a very sensitive function of base to emitter voltage, Q4 provides substantial amplification of small variations in D6 current flow and therefore bias voltage level. The overall result is to regulate the bias voltage applied to Zener diode D6. Output is taken from the junction of the emitter of Q3 and D6 since that point is well regulated by the combination of Zener diode breakdown voltage combined with the amplification provided by Q4. In addition to good voltage regulation a the junction of the emitter of Q3 and D6, the output is very tolerant of load current demand since the conductivity of Q3 will be changed by shifts in the operating point of Q4. Due to amplification by Q3 and Q4, the circuit can drive a range of load resistances. Tolerable load resistances above 1000 ohms and less than 200 ohms. The regulator has the advantage of delivering only the current needed to operate the load while consuming only moderate bias current. Further, bias current is only drawn during delivery of the stimulation pulse which drops to zero when no stimulation is delivered. As a comparison, a simple series resistance biased Zener diode requires enough excess current to deliver a stimulation pulse and still maintain adequate Zener bias. As a further comparison, conventional integrated circuit regulators, such as three terminal regulators are not designed to well regulate and respond quickly to short input pulses. Experiment shows that three-terminal regulators exhibit significant output overshoot and ramp-up time upon application of an input pulse. This can be addressed by applying a constant bias to a regulator circuit or even moving the regulator before the output switching stage but this will be at the cost of constant current drain and subsequently reduced range.
The implanted electronics unit may be used to manage the loss of control and power signals. With this design, more than enough stimulation power is stored in C3 to supply multiple delivered stimulation pulses. This design is intended to ensure that the voltage drop is minimal on any individual pulse. One of the consequences is that when signal is lost, the circuit treats the condition as a commanded delivery of stimulation and will apply a single, extended duration, energy pulse until the full stored capacity of C3 is empty. An alternative method may be to use an indirect control modulation to command delivery of a nerve stimulation pulse through logic and provide for a time-out that limits pulse duration.
To stimulate tissue, a modified output stage may be used to mitigate electrode corrosion and establish balanced charging. The output stage is illustrated inFIG. 52G and includes a capacitive coupling between the ground side of the stimulator and tissue interface in addition to a shunt from the active electrode to circuit ground for re-zeroing the output coupling capacitor when an output pulse is not being actively delivered.
Description of Alternative Screening Methods
Screening generally refers to selecting patients that will be responsive to the therapy, namely neurostimulation of the upper airway dilator nerves and/or muscles such as the hypoglossal nerve that innervates the genioglossus. Screening may be based on a number of different factors including level of obstruction and critical collapse pressure (Pcrit) of the upper airway, for example. Because stimulation of the hypoglossal nerve affects the genioglossus (base of tongue) as well as other muscles, OSA patients with obstruction at the level of the tongue base and OSA patients with obstruction at the level of the palate and tongue base (collectively patients with tongue base involvement) may be selected. Because stimulation of the hypoglossal nerve affects upper airway collapsibility, OSA patients with airways that have a low critical collapse pressure (e.g., Pcrit of less than about 5 cm water) may be selected. Pcrit may be measured using pressure transducers in the upper airway and measuring the pressure just prior to an apnea event (airway collapse). Alternatively, a surrogate for Pcrit such as CPAP pressure may be used. In this alternative, the lowest CPAP pressure at which apnea events are mitigated may correlate to Pcrit.
The critical collapse pressure (Pcrit) may be defined as the pressure at which the upper airway collapses and limits flow to a maximal level. Thus, Pcrit is a measure of airway collapsibility and depends on the stability of the walls defining the upper airway as well as the surrounding pressure. Pcrit may be more accurately defined as the pressure inside the upper airway at the onset of flow limitation when the upper airway collapses. Pcrit may be expressed as:
Pcrit=Pin−Pout
where
Pin=pressure inside the upper airway at the moment of airway collapse; and
Pout=pressure outside the upper airway (e.g., atmospheric pressure).
Other screening methods and tools may be employed as well. For example, screening may be accomplished through acute testing of tongue protruder muscle contraction using percutaneous fine wire electrodes inserted into the genioglossus muscle, delivering stimulus and measuring one or more of several variables including the amount of change in critical opening pressure, the amount of change in airway caliber, the displacement of the tongue base, and/or the retraction force of the tongue (as measured with a displacement and/or force gauge). For example, a device similar to a CPAP machine can be used to seal against the face (mask) and control inlet pressure down to where the tongue and upper airway collapse and occlude during inspiration. This measurement can be repeated while the patient is receiving stimulation of the geneoglossus muscle (or other muscles involved with the patency of the upper airway). Patients may be indicated for the stimulation therapy if the difference in critical pressure (stimulated vs. non-stimulated) is above a threshold level.
Similarly, a flexible optical scope may be used to observe the upper airway, having been inserted through the mask and nasal passage. The difference in upper airway caliber between stimulation and non-stimulation may be used as an inclusion criterion for the therapy. The measurement may be taken with the inlet air pressure to the patient established at a pre-determined level below atmospheric pressure to better assess the effectiveness of the stimulation therapy.
Another screening technique involves assessing the protrusion force of the tongue upon anterior displacement or movement of the tongue with and without stimulation while the patient is supine and (possibly) sedated or asleep. A minimum increase in protrusion force while under stimulation may be a basis for patient selection.
For example, with reference toFIG. 53, a non-invasive oral appliance530 may be worn by the patient during a sleep study that can directly measure the protrusion force of the tongue as a basis for patient selection. The oral appliance530 may include a displacement probe532 for measuring tongue movement protrusion force by deflection (D). The oral appliance530 may also include aforce sensor534 for measuring the force (F) applied by protrusion of the tongue. The sensors in the displacement probe532 and theforce sensor534 may be connected to measurement apparatus by wires536.
FIG. 54 illustrates another example of a non-invasiveoral appliance540 that may be worn by the patient during a sleep study to directly measure the protrusion force of the tongue as a basis for patient selection. Theoral appliance540 includes adisplacement sensor542 for measuring tongue movement and a force sensor for measuring tongue protrusion force. The displacement sensor and the force sensor may be connected to measurement apparatus by wires546.
Oral appliances530 and540 could be worn during a sleep study and would measure the tongue protrusion force during (and just prior to) an apnea event when the protruder muscle tone is presumed to be inadequate to maintain upper airway patency. The protrusion force measured as the apnea is resolved by the patient will increase as the patient changes sleep state and the airway again becomes patent. The force difference may be used as a basis for patient selection.
Another screening technique involves the use of an oral appliance with sub-lingual surface electrodes contacting the base of the tongue or fine wire electrodes inserted into the genioglossus muscle to stimulate the tongue protruder muscle(s) synchronous with respiration during a sleep study. The oral appliance may be fitted with a drug delivery system (e.g., drug eluting coating, elastomeric pump, electronically controlled pump) for topical anesthesia to relieve the discomfort of the electrodes.
For example, with reference toFIG. 55, anoral appliance550 includes a pair of small needle intramuscular electrodes552 that extend into the genioglossus. The electrodes552 are carried by flexible wires554 and may be coupled to an external pulse generator (not shown) by wires556. The electrodes552 may be supported by a drug (e.g., anesthetic) eluting polymeric member558.
Alternatively, with reference toFIG. 56, an oral appliance560 includes acathode electrode562 guarded by twoanode electrodes564 carried by a soft extension565 that extends under the tongue. Thesurface electrodes562 and564 contact the floor of the mouth under the tongue to indirectly stimulate the genioglossus. Theelectrodes562 and564 may be coupled to an external pulse generator (not shown) by wires566. The extension565 may incorporate holes568 through which a drug (e.g., anesthetic) may be eluted.
Oral appliances550 and560 may be used during a sleep study and stimulation of the target tissue can be performed synchronous with respiration and while inlet airflow pressure can be modulated. The ability to prevent apneas/hypopneas can be directly determined. Also the critical opening pressure with and without stimulation can be determined. Alternatively or in addition, the intramuscular or surface electrodes may be used to measure genioglossus EMG activity, either with or without stimulation. On any of theses bases, patient selection may be made.
Patient selection may also be applied to the respiratory sensors to determine if the respiratory sensors will adequately detect respiration for triggering stimulation. For example, in the embodiment wherein bio-Z is used to detect respiration using an implantedlead70, skin surface or shallow needle electrodes may be used prior to implantation to determine if the signal will be adequate. This method may also be sued to determine the preferred position of the electrodes (i.e., optimal bio-Z vector). This may be done while the patient is sleeping (i.e., during a sleep study) or while the patient is awake.
Description of Alternative Intra-Operative Tools
Intra-operatively, it may be desirable to determine the correct portion of the nerve to stimulate in order to activate the correct muscle(s) and implant the nerve cuff electrode accordingly. Determining the correct position may involve stimulating at different locations along the length or circumference of the nerve and observing the effect (e.g., tongue protrusion). In addition or in the alternative, and particularly in the case of field steering where multiple combinations of electrode contacts are possible, it may be desirable to determine optimal electrode or filed shape combinations.
An example of an intra-operativestimulating tool570 is shown inFIGS. 57A and 57B. In this embodiment, thetool570 includes afirst shaft571 with a distal half-cuff573.Tool570 further includes asecond shaft575 with a proximalmovable collar574 and a distal half-cuff575.Stimulating tool570 includes multiple electrodes572 on half-cuff573 and/or half-cuff575 that may be arranged in an array or matrix as shown inFIG. 57C, which is a view taken along line A-A inFIG. 57B. The half-cuffs573 and575 may be longitudinally separated for placement about a nerve and subsequently closed such that the half-cuffs573 and575 gently grasp the nerve. Theelectrodes575 may be sequenced through a series of electrode/field shape combinations to optimize (lower) the critical opening pressure, airway caliber, tongue protrusion force or other acute indicia of therapeutic efficacy.
Thetool570 may be part of an intra-operative system including: (1)tool570 or other tool with one or more stimulating electrodes that are designed to be easily handled by the surgeon during implant surgery; (2) an external pulse generator which triggers off of a respiration signal; (3) a feedback diagnostic device that can measure critical closing pressure intra-operatively; and (4) an algorithm (e.g., firmware or software in the programmer) that is design to automatically or manually sequence through a series of electrode configurations that will identify the best placement of electrode cuffs on the nerves and configuration of electrode polarity and amplitude settings. Information from the intra-operative system may greatly speed the process of identifying where to place the electrode cuff(s) on the hypoglossal nerve and what field steering may be optimal or necessary to provide efficacy.
In certain circumstances, such as, when treating a child or a small adult, it may be difficult to implant a nerve cuff electrode of the present disclosure about a nerve in a patient's body. Accordingly, it may be desirable to provide a tool capable of facilitating temporary expansion of a nerve cuff electrode of the present disclosure, so as to slip the nerve cuff electrode around a patient's nerve. Turning now toFIGS. 58A-58B, there is depicted atool5800 for temporarily expanding a nerve cuff electrode in accordance with the principles of the present disclosure.Tool5800 may include a substantially scissor-like configuration having afirst element5801 and asecond element5802 pivotably secured together by a suitable fastener, such as, for example, pivot pin5803, acting as a fulcrum.Elements5801 and5802 may be substantially similar to each other or may differ as necessary. In the depicted embodiment,elements5801 and5802 may include levers having distal effecting portions5804,5805 andproximal actuating portions5806,5807.
Proximal actuating portions5806,5807 may be of any suitable length and may be connected to respective handles (not shown), which may be used to operatetool5800. Alternatively,proximal actuating portions5806,5807 themselves may be used to operatetool5800. Distal effecting portions5804,5805 may include any suitable configuration to achieve the desired effect. For example, each portion5804,5805 may include a substantially curved configuration. Additionally, a distal end of each portion5804,5805 may be provided with a fastening mechanism, such as, for example, hook-like projection5804a,5805a, for facilitating connection oftool5800 to a nerve cuff electrode. As shown inFIGS. 58A-58B, hook-like projections5804a,5805a may be configured to be disposed in differing parallel planes, such that projections5804a,5805a may be spaced (offset) horizontally from one another. In use, distal effecting portions5804,5805 may be opened and closed asproximal actuating portions5806,5807 may be rotated about pivot pin5803.
In embodiments wheretool5800 may be used to temporarily expand a nerve cuff electrode for implantation purposes, the nerve cuff electrode, e.g.,nerve cuff electrode5810, may be provided with one more geometric configurations for facilitation connection withtool5800. In the depicted embodiment,nerve cuff electrode5810 may be provided withextensions5811,5812 for facilitating connection withtool5800. Eachextension5811,5812 may be provided with openings5811a,5812a, respectively, for receiving hook-like projections5804a,5805a, so as to operably couple nerve cuff electrode5811 withtool5800.
Description of Miscellaneous Alternatives
The implanted neurostimulation system may be configured so that stimulation of the nerve is set at a relatively low level (i.e., low voltage amplitude, narrow pulse width, lower frequency) so as to maximize battery life of the INS and to minimize the chances that the electrical stimulation will cause arousal from sleep. If apneas/hypopneas are detected, then the electrical stimulation can be increased progressively until the apneas/hypopneas are no longer detected, up to a maximum pre-set stimulation level. This auto titration may automatically be reset to the low level after the patient is awakened and sits up (position detector) or manually reset using the patient controller. The stimulation level may be automatically reduced after a period of time has elapsed with no (or few) apneas/hypopneas detected.
The stimulation level (i.e., voltage amplitude, pulse width, frequency) may be adjusted based on changes in respiration rate. Respiration rate or patterns of rate change may be indicative of sleep state. A different power level based on sleep state may be used for minimal power consumption, minimal unwanted stimulation (sensory response), etc., while providing adequate efficacy.
The electrical field shape used to stimulate the target nerve can be changed while the system is proving therapy based on feedback indicating the presence (or lack) of apneas/hypopneas. The electrical field shape for an implanted system can be changed by adjusting the polarity, amplitude and other stimulation intensity parameters for each of the electrodes within the nerve stimulating cuff. An algorithm within the INS may change the currently operating electrical field shape if the presence of apneas/hypopneas is detected, and then wait a set period of time to determine if the new configuration was successful in mitigating the apneas/hypopneas before adjusting the field shape again. Additionally, the system may be designed to keep a log of the most successful stimulation patterns and when they were most likely to be effective. This may allow the system to “learn” which settings to be used during what part of the night, for example, or with specific breathing patterns or cardiac signal patterns or combinations thereof.
The proportion of stimulation intensity of two electrode cuffs used to stimulate a nerve can be modulated while the system is providing therapy based on feedback indicating the presence (or lack) of apneas/hypopneas. For example, one nerve stimulating electrode cuff may be place on the more proximal section of the hypoglossal nerve, while a second is placed more distally. The proximal cuff will be more likely to stimulate branches of the hypoglossal nerve going to muscles in the upper airway involved with tongue or hyoid retrusion while the more distal electrode cuff will more likely stimulate only the muscles involved with tongue/hyoid protrusion. Research suggests that to best maintain upper airway patency, stimulating both protrudes and retruders (in the right proportion) may be more effective that stimulating protruders alone. Software within the INS may change the currently operating proportion of electrical stimulation going to the distal electrode cuff in proportion to that going to the proximal cuff based on the presence of apneas/hypopneas detected. The system may then wait a set period of time to determine if the new configuration was successful in mitigating the apneas/hypopneas before adjusting the system again. Additionally, the system software may be designed to keep a log of the most successful stimulation proportion and when they were most likely to be effective. This may allow the system to “learn” which settings to be used during what part of the night, for example, or with specific breathing patterns or cardiac signal patterns or combinations thereof.
The system described above may modulate electrical stimulation intensity proportion based on electromyogram (EMG) feedback from the muscles in the upper airway being stimulated or others in the area. This feedback may be used to determine the correct proportion of stimulation between protruders and retruders. The correct ratio of EMG activity between retruders and protruders may be determined during a sleep study for an individual, may be determined to be a constant for a class of patients or may be “learned” my the implanted system by using the detection of apneas/hypopneas as feedback.
A library of electrical stimulation parameter settings can be programmed into the INS. These settings listed in the library may be selected by the patient manually using the patient programmer based on, for example: (1) direct patient perception of comfort during stimulation; (2) a log of the most successful settings compiled by the software in the INS (assumes apnea/hypopnea detection capability); (3) a sleep physician's or technician's assessment of the most effective stimulation as determined during a sleep study; and/or (4) a list of the most effective parameters produced for a particular class of patient or other.
The electrical stimulation parameters described above may be adjusted based on patient position as detected by a position sensor within the INS. The best setting for a given position may be determined by, for example: (1) a log of the most successful settings compiled or learned by the software in the INS (assumes apnea/hypopnea detection capability); (2) a sleep physician's or technician's assessment of the most effective stimulation as determined during a sleep study; and/or (3) a list of the most effective parameters produced for a particular class of patient or other.
To avoid fatigue using a normal duty cycle or to extend the time that the upper airway is opened through neurostimulation, different parts of the genioglossus muscle and/or different muscles involved with establishing patency of the upper airway can be alternately stimulated. For example, using two or more nerve or muscle electrode cuffs, the left and right side genioglossus muscles can be alternately stimulated, cutting the effective duty cycle on each muscle in half. In addition, different protruder muscles on the ipsilateral side such as the geniohyoid and the genioglossus muscle can be alternately stimulated to the same effect. This may also be accomplished through one electrode cuff using field steering methods that selectively stimulated the fascicles of the hypoglossal nerve going to one group of protruders alternating with stimulating the fascicles leading to a different protruder muscle group. This method may also be used to alternately stimulate one group of muscle fibers within the genioglossus muscle with the compliment of muscle fibers in the same muscle group.
To increase the ability of the upper airway to open during a (sensed) apnea/hypopnea through neurostimulation, different parts of the genioglossus muscle and/or different muscles involved with establishing patency of the upper airway can be simultaneously stimulated. For example, using two or more nerve or muscle electrode cuffs, the left and right side genioglossus muscles can be simultaneously stimulated, greatly increasing the protrusion forces. In addition, different protruder muscles on the ipsilateral side such as the geneohyoid and the genioglossus muscle can be simultaneously stimulated to the same effect. This may also be accomplished through one electrode cuff using field steering methods that selectively stimulated the fascicles of the hypoglossal nerve going to one group of protruders simultaneously with stimulating the fascicles leading to a different protruder muscle group. This may be achieved with one electrode cuff using field steering on a more proximal location on the hypoglossal nerve or two or more electrode cuffs, one on each branch going to a muscle involved with maintaining muscle patency.
A sensor inside the INS (or elsewhere in system implanted) may detect body position and automatically shut off stimulation when patient sits up or stands up. This will prevent unwanted stimulation when patient is no longer sleeping. The device may automatically restart the stimulation after the sensor indicates the patient is again horizontal, with or without a delay. The system may also be configured so that the stimulation can only be restarted using the patient controller, with, or without a delay.
The respiration signal using impedance and/or EMG/ENG are easily capable of determining heart rate. The stimulation may be interrupted or turned off when the heart rate falls outside out a pre-determined acceptable range. This may be an effective safety measure that will decrease the chance that hypoglossal nerve stimulation will interfere with mitigating physiological processes or interventional emergent medical procedures.
Respiration waveforms indicating apneas/hypopneas or of other clinical interest may be recorded and automatically telemetered to a bed-side receiver unit or patient programmer. Respiration waveforms indicating frequent apneas/hypopneas, abnormal breathing patterns, irregular heart rate/rhythm may be recorded and automatically telemetered to a bed-side deceiver unit or patient programmer causing an alarm to be issued (audible/visible). The INS status such as low battery or system malfunction may also trigger an alarm.
Electrical stimulation intensity could be ramped up for each respiration cycle by increasing amplitude or pulse width from 0 to a set point to prevent sudden tongue protrusion or sudden airway opening causing the patient to wake up. During inspiration, the system may deliver approximately 30 pulses per second for a length of time of one to one and one half seconds, totaling between about 30 and 45 pulses per respiration cycle. Prior to delivery of these 30 to 45 pulses, amplitude of each individual therapy pulse (in an added group of pulses) could be ramped up from 0 to a set point at a rate of <10% of the amplitude intended for the active duty cycle or 200 mS, whichever is less. The pulse width of each individual therapy pulse could be ramped up from 0 to a set point at a rate of <10% of the active duty cycle or 200 mS, whichever is less. Each of these ramp methods would require a predictive algorithm that would stimulate based on the previous inspiration cycle.
Nerves innervating muscles that are involved with inspiration, such as the hypoglossal nerve, have been shown to have greater electrical activity during apnea or hypopnea. This signal cannot be easily measured while simultaneously stimulating the same nerve. One method of stimulating and sensing using the same lead is to interleave a sensing period within the stimulation pulse bursts during the duty cycle. In other words, the sensing period may occur between pulses within the stimulation pulse train. This approach may be used with electrodes/leads that directly stimulate and alternately sense on a nerve involved with inspiration or on a muscle involved with inspiration or a combination of the two. The approach may allow sensing of apnea/hypopnea, as well as therapeutic stimulation.
From the foregoing, it will be apparent to those skilled in the art that the present invention provides, in exemplary non-limiting embodiments, devices and methods for nerve stimulation for OSA therapy. Further, those skilled in the art will recognize that the present invention may be manifested in a variety of forms other than the specific embodiments described and contemplated herein. Accordingly, departures in form and detail may be made without departing from the scope and spirit of the present invention as described in the appended claims.

Claims (25)

What is claimed is:
1. A method of maintaining patency of an upper airway of a patient to treat obstructive sleep apnea, the method comprising:
sensing a biological parameter indicative of respiration, wherein the biological parameter includes impedance;
analyzing the biological parameter to identify onsets of expiration;
calculating a respiratory period from the onsets of expiration;
predicting an onset of a future expiratory phase; and
beginning stimulation of a nerve a fraction of the calculated respiratory period before the onset of the future expiratory phase, and continuing stimulation of the nerve during an entire inspiratory phase, wherein the method is performed without identifying an onset of the inspiratory phase.
2. The method ofclaim 1, wherein the nerve is an internal branch of a superior laryngeal nerve.
3. The method ofclaim 1, further comprising:
implanting an impedance sensor within the patient, wherein the impedance sensor is coupled to an electrical stimulator by a sensing lead.
4. The method ofclaim 1, wherein beginning stimulation of the nerve includes delivering electrical stimulation to one of a hypoglossal nerve and a glossopharyngeal nerve.
5. The method ofclaim 4, further comprising delivering stimulation to a portion of a superior laryngeal nerve concurrently with the stimulation delivered to the one of a hypoglossal nerve and a glossopharyngeal nerve.
6. The method ofclaim 1, further comprising: steering an electrical field of a nerve cuff to stimulate only afferent fibers of the nerve.
7. The method ofclaim 1, wherein the step of beginning stimulation of a nerve includes delivering stimulation to only afferent fibers of an internal branch of a superior laryngeal nerve.
8. The method ofclaim 1, wherein the stimulation is delivered via a nerve cuff connected to an electrical stimulator via a stimulation lead including a portion having a serpentine configuration.
9. The method ofclaim 8, wherein the stimulation lead includes a portion configured to be secured to a body structure other than a nerve.
10. The method ofclaim 8, wherein the nerve cuff includes a plurality of electrodes in direct contact with the nerve.
11. The method ofclaim 1, further comprising:
an electrode sensor for wherein the step of sensing the biological parameter, wherein the electrode sensor is performed via an electrode sensor coupled to sensing circuitry of an electrical stimulator,
wherein stimulation of the nerve includes delivering an electrical stimulation to a glossopharyngeal nerve via a nerve cuff having a plurality of electrodes, wherein the nerve cuff is connected to-the to the electrical stimulator by a stimulation lead, and wherein a portion of the stimulation lead is configured to elongate in response to movement by the patient.
12. The method ofclaim 11, wherein the stimulation lead further includes a portion configured to be secured to a body structure other than a nerve.
13. The method ofclaim 1, wherein the stimulation is delivered to the nerve via a nerve cuff connected to an electrical stimulator, the nerve cuff comprising:
a base member extending from a first side wall to a second side wall and having a top wall and a bottom wall;
a first member extending from the first side wall;
a second member extending from the second side wall; and
a third member having a first end fixedly engaged to the first side wall adjacent the first member, wherein the third member extends over the top wall of the base member, the second member extends over the top wall of the base member, and the first member, the second member, and the third member define a lumen.
14. The method ofclaim 13, wherein the third member is capable of transitioning between a first position, prior to positioning of the electrode cuff about a nerve, and a second position subsequent to the positioning of the electrode cuff about the nerve, wherein the third member is positioned a first distance above the top wall of the base member in the first position, and the third member is positioned a second distance smaller than the first distance above the top wall of the base member in the second position.
15. The method ofclaim 13, wherein the second member is capable of transitioning between a first position, prior to positioning of the electrode cuff about a nerve, and a second position subsequent to the positioning of the electrode cuff about the nerve, wherein the second member is positioned a first distance above the top wall of the base member in the first position, and the second member is positioned a second distance, greater than the first distance, above the top wall of the base member in the second position.
16. The method ofclaim 13, wherein the second member has a first thickness at a first end of the second member and a second thickness, less than the first thickness, at a second end.
17. A method of treating obstructive sleep apnea by innervating a mechanoreceptor within a patient's upper airway via stimulating a superior laryngeal nerve including both afferent and efferent fibers, the method comprising:
chronically implanting a nerve cuff adjacent a portion of a superior laryngeal nerve:;
sensing a biological parameter indicative of respiration, wherein the biological parameter includes impedance;
analyzing the sensed biological parameter to identify onsets of expiration;
calculating a respiratory period from the onsets of expiration;
predicting the onset of a future expiratory phase; and
beginning stimulation of the superior laryngeal nerve a fraction of the calculated respiratory period before the onset of the future expiratory phase, and continuing stimulation of the superior laryngeal nerve during an entire inspiratory phase, wherein the method is performed without identifying an onset of the inspiratory phase.
18. The method ofclaim 17, further comprising:
delivering an electrical stimulation to one of a hypoglossal nerve and a glossopharyngeal nerve simultaneously with the stimulation to the superior laryngeal nerve.
19. The method ofclaim 17, further comprising:
steering an electrical field of the nerve cuff to stimulate only the afferent fibers of an internal branch of the superior laryngeal nerve.
20. The method ofclaim 17, wherein the nerve cuff includes a plurality of electrodes in direct contact with a surface of the superior laryngeal nerve.
21. A method of treating obstructive sleep apnea, the method comprising:
chronically implanting a nerve cuff adjacent a portion of a superior laryngeal nerve;
sensing a biological parameter indicative of respiration, wherein the biological parameter includes impedance;
analyzing the biological parameter to identify onsets of expiration;
calculating a respiratory period from the onsets of expiration;
predicting an onset of a future expiratory phase; and
beginning stimulation of the superior laryngeal nerve a fraction of the calculated respiratory period before the onset of the future expiratory phase, and continuing stimulation of the superior laryngeal nerve during an entire inspiratory phase, wherein the method is performed without identifying an onset of the inspiratory phase.
22. A method of treating obstructive sleep apnea, the method comprising:
sensing a biological parameter indicative of respiration, wherein the biological parameter includes impedance;
analyzing the biological parameter to identify onsets of expiration;
calculating a respiratory period from the onsets of expiration;
predicting an onset of a future expiratory phase; and
beginning stimulation of a nerve a fraction of the calculated respiratory period before the onset of the future expiratory phase, and continuing stimulation of the nerve during an entire inspiratory phase, wherein the method is performed without identifying an onset of the inspiratory phase.
23. The method of claim 1, further comprising steering an electrical field of a nerve cuff to stimulate fibers of the nerve, wherein a majority of the stimulated fibers of the nerve comprises afferent fibers.
24. The method of claim 1, wherein beginning stimulation of the nerve includes delivering stimulation to fibers of an internal branch of a superior laryngeal nerve, and wherein a majority of the fibers to which stimulation is delivered comprises afferent fibers.
25. The method of claim 17, further comprising steering an electrical field of the nerve cuff to stimulate fibers of an internal branch of the superior laryngeal nerve, wherein a majority of the stimulated fibers of the nerve comprises afferent fibers.
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* Cited by examiner, † Cited by third party
Publication numberPriority datePublication dateAssigneeTitle
US12226223B2 (en)2011-09-062025-02-18Resmed Sensor Technologies LimitedMulti-modal sleep system

Families Citing this family (379)

* Cited by examiner, † Cited by third party
Publication numberPriority datePublication dateAssigneeTitle
US6907295B2 (en)2001-08-312005-06-14Biocontrol Medical Ltd.Electrode assembly for nerve control
US20090005845A1 (en)*2007-06-262009-01-01Tamir Ben DavidIntra-Atrial parasympathetic stimulation
US8565896B2 (en)*2010-11-222013-10-22Bio Control Medical (B.C.M.) Ltd.Electrode cuff with recesses
US8615294B2 (en)2008-08-132013-12-24Bio Control Medical (B.C.M.) Ltd.Electrode devices for nerve stimulation and cardiac sensing
US7778711B2 (en)*2001-08-312010-08-17Bio Control Medical (B.C.M.) Ltd.Reduction of heart rate variability by parasympathetic stimulation
US7904176B2 (en)*2006-09-072011-03-08Bio Control Medical (B.C.M.) Ltd.Techniques for reducing pain associated with nerve stimulation
US7035690B2 (en)2002-11-152006-04-25Medtronic, Inc.Human-implantable-neurostimulator user interface having multiple levels of abstraction
US8880192B2 (en)2012-04-022014-11-04Bio Control Medical (B.C.M.) Ltd.Electrode cuffs
US8718791B2 (en)*2003-05-232014-05-06Bio Control Medical (B.C.M.) Ltd.Electrode cuffs
US20050149132A1 (en)2003-12-242005-07-07Imad LibbusAutomatic baroreflex modulation based on cardiac activity
US10912712B2 (en)2004-03-252021-02-09The Feinstein Institutes For Medical ResearchTreatment of bleeding by non-invasive stimulation
US11207518B2 (en)*2004-12-272021-12-28The Feinstein Institutes For Medical ResearchTreating inflammatory disorders by stimulation of the cholinergic anti-inflammatory pathway
WO2007098200A2 (en)*2006-02-162007-08-30Imthera Medical, Inc.An rfid-based apparatus, system, and method for therapeutic treatment of obstructive sleep apnea
US8380321B2 (en)2006-02-242013-02-19Medtronic, Inc.Programming interface with a cross-sectional view of a stimulation lead with complex electrode array geometry
US8612024B2 (en)2006-02-242013-12-17Medtronic, Inc.User interface with 3D environment for configuring stimulation therapy
US9020597B2 (en)2008-11-122015-04-28Endostim, Inc.Device and implantation system for electrical stimulation of biological systems
US8437843B1 (en)2006-06-162013-05-07Cleveland Medical Devices Inc.EEG data acquisition system with novel features
US20150224310A1 (en)2006-10-092015-08-13Endostim, Inc.Device and Implantation System for Electrical Stimulation of Biological Systems
US9724510B2 (en)2006-10-092017-08-08Endostim, Inc.System and methods for electrical stimulation of biological systems
US9345879B2 (en)2006-10-092016-05-24Endostim, Inc.Device and implantation system for electrical stimulation of biological systems
US11577077B2 (en)2006-10-092023-02-14Endostim, Inc.Systems and methods for electrical stimulation of biological systems
US8855771B2 (en)2011-01-282014-10-07Cyberonics, Inc.Screening devices and methods for obstructive sleep apnea therapy
AU2007313319B2 (en)2006-10-132012-03-22Cyberonics, Inc.Obstructive sleep apnea treatment devices, systems and methods
US9913982B2 (en)*2011-01-282018-03-13Cyberonics, Inc.Obstructive sleep apnea treatment devices, systems and methods
US9205262B2 (en)*2011-05-122015-12-08Cyberonics, Inc.Devices and methods for sleep apnea treatment
US9744354B2 (en)2008-12-312017-08-29Cyberonics, Inc.Obstructive sleep apnea treatment devices, systems and methods
US9186511B2 (en)2006-10-132015-11-17Cyberonics, Inc.Obstructive sleep apnea treatment devices, systems and methods
US20110009925A1 (en)*2006-10-172011-01-13Cochlear LimitedTranscutaneous receiving antenna device for implant
US8798759B2 (en)*2006-12-062014-08-05Medtronic, Inc.User interface with toolbar for programming electrical stimulation therapy
CA2748056A1 (en)*2006-12-152008-06-19Nasophlex B.V.Resuscitation device and method for resuscitation
US7890178B2 (en)*2006-12-152011-02-15Medtronic Xomed, Inc.Method and apparatus for assisting deglutition
US8082034B2 (en)2007-01-262011-12-20Medtronic, Inc.Graphical configuration of electrodes for electrical stimulation
US9072897B2 (en)2007-03-092015-07-07Mainstay Medical LimitedSystems and methods for restoring muscle function to the lumbar spine
US11679262B2 (en)2007-03-092023-06-20Mainstay Medical LimitedSystems and methods for restoring muscle function to the lumbar spine
EP2125100B1 (en)2007-03-092021-08-25Mainstay Medical LimitedMuscle stimulator
US10925637B2 (en)2010-03-112021-02-23Mainstay Medical LimitedMethods of implanting electrode leads for use with implantable neuromuscular electrical stimulator
US11679261B2 (en)2007-03-092023-06-20Mainstay Medical LimitedSystems and methods for enhancing function of spine stabilization muscles associated with a spine surgery intervention
US11331488B2 (en)2007-03-092022-05-17Mainstay Medical LimitedSystems and methods for enhancing function of spine stabilization muscles associated with a spine surgery intervention
US10426399B1 (en)*2007-06-082019-10-01Cleveland Medial Devices Inc.Method and device for in-home sleep and signal analysis
US9202008B1 (en)*2007-06-082015-12-01Cleveland Medical Devices Inc.Method and device for sleep analysis
AU2008279121B2 (en)*2007-07-242013-09-19Boston Scientific Scimed, Inc.System and method for controlling power based on impedance detection, such as controlling power to tissue treatment devices
US8391970B2 (en)*2007-08-272013-03-05The Feinstein Institute For Medical ResearchDevices and methods for inhibiting granulocyte activation by neural stimulation
US20100198103A1 (en)2007-10-092010-08-05Imthera Medical, Inc.System and method for neural stimulation
US20170188940A9 (en)2007-11-262017-07-06Whispersom CorporationDevice to detect and treat Apneas and Hypopnea
US7954494B1 (en)2008-03-262011-06-07Connor Robert ADevice with actively-moving members that hold or move the tongue
US9211409B2 (en)*2008-03-312015-12-15The Feinstein Institute For Medical ResearchMethods and systems for reducing inflammation by neuromodulation of T-cell activity
US9662490B2 (en)2008-03-312017-05-30The Feinstein Institute For Medical ResearchMethods and systems for reducing inflammation by neuromodulation and administration of an anti-inflammatory drug
EP2310084B1 (en)*2008-05-022016-03-23Medtronic, Inc.Electrode lead system
WO2009134434A1 (en)2008-05-022009-11-05Dymedix CorporationAgitator to stimulate the central nervous system
US8340785B2 (en)*2008-05-022012-12-25Medtronic, Inc.Self expanding electrode cuff
EP3708219B1 (en)*2008-05-152022-08-03Inspire Medical Systems, Inc.Apparatus for sensing respiratory pressure in an implantable stimulation system
EP2320790B1 (en)2008-06-062017-10-04Covidien LPSystems for determining patient effort and/or respiratory parameters in a ventilation system
NL2001698C2 (en)2008-06-182009-12-22Nasophlex B V Cardioverter / defibrillator.
WO2009154456A1 (en)*2008-06-182009-12-23Kerphos B.V.A flexible electronic system for producing a stimulation signal to the human body.
NL2001697C2 (en)2008-06-182009-12-22Nasophlex B V Nose stimulator for producing a stimulation signal to a nose.
NL2001694C2 (en)*2008-06-182009-12-22Nasophlex B V Ear stimulator for producing a stimulation signal to an ear.
WO2010006218A2 (en)*2008-07-112010-01-14Don HeadleySleep apnea device and method
US7803021B1 (en)2008-07-212010-09-28Boston Scientific Neuromodulation CorporationImplantable electrical stimulation systems with leaf spring connective contacts and methods of making and using
US20100057148A1 (en)*2008-08-222010-03-04Dymedix CorporationStimulus timer for a closed loop neuromodulator
DK2346395T3 (en)*2008-09-222018-06-06Cheetah Medical Inc SYSTEM AND PROCEDURE FOR DETERMINING BLOOD FLOW
JP5547200B2 (en)*2008-10-012014-07-09インスパイア・メディカル・システムズ・インコーポレイテッド Transvenous treatment to treat sleep apnea
BRPI0920548B8 (en)2008-10-092021-06-22Imthera Medical Inc device to control the position of a patient's tongue
AU2014253460B2 (en)*2008-10-092017-02-02Imthera Medical, Inc.Method of stimulating a hypoglossal nerve for controlling the position of a patient's tongue
US8616208B2 (en)*2008-10-292013-12-31Industrial Technology Research InstituteOral appliance with auto negative pressure control and method thereof
US8548593B2 (en)*2008-11-102013-10-01Cardiac Pacemakers, Inc.Distal end converter for a medical device lead
CA2744269C (en)*2008-11-182020-04-14Willard WilsonDevice and method for detecting sleep apnea events by monitoring the internal branch of the superior laryngeal nerve
EP2355893B1 (en)2008-11-182013-12-25Setpoint Medical CorporationDevices for optimizing electrode placement for anti-inflamatory stimulation
EP3184045B1 (en)*2008-11-192023-12-06Inspire Medical Systems, Inc.System treating sleep disordered breathing
US8515520B2 (en)*2008-12-082013-08-20Medtronic Xomed, Inc.Nerve electrode
US9486628B2 (en)2009-03-312016-11-08Inspire Medical Systems, Inc.Percutaneous access for systems and methods of treating sleep apnea
US20100256696A1 (en)*2009-04-072010-10-07Boston Scientific Neuromodulation CorporationAnchoring Units For Implantable Electrical Stimulation Systems And Methods Of Making And Using
WO2010121170A1 (en)2009-04-162010-10-21Boston Scientific Neuromodulation CorporationDeep brain stimulation current steering with split electrodes
US9211410B2 (en)2009-05-012015-12-15Setpoint Medical CorporationExtremely low duty-cycle activation of the cholinergic anti-inflammatory pathway to treat chronic inflammation
US8996116B2 (en)2009-10-302015-03-31Setpoint Medical CorporationModulation of the cholinergic anti-inflammatory pathway to treat pain or addiction
EP2435129B1 (en)2009-05-262015-07-01Cardiac Pacemakers, Inc.Helically formed coil for a neural cuff electrode
WO2010144578A2 (en)*2009-06-092010-12-16Setpoint Medical CorporationNerve cuff with pocket for leadless stimulator
US8545231B2 (en)*2009-06-252013-10-01Charles Richard LloydObstructive sleep apnea demonstration model device
EP2459274B1 (en)*2009-07-302015-11-11Richard NorthModular electrode and insertion tool
CA2770151A1 (en)*2009-08-052011-02-10Ndi Medical, LlcSystems and methods for maintaining airway patency
WO2011028763A2 (en)*2009-09-012011-03-10Setpoint Medical CorporationPrescription pad for treatment of inflammatory disorders
US8160712B1 (en)*2009-09-232012-04-17Marcy FreedApparatus and method for treating sleep apnea
US9415216B2 (en)2009-10-202016-08-16Nyxoah SADevices for treatment of sleep apnea
US10806926B2 (en)*2009-10-202020-10-20Man & Science SaImplantable electrical stimulator
US9409013B2 (en)2009-10-202016-08-09Nyxoah SAMethod for controlling energy delivery as a function of degree of coupling
US9950166B2 (en)2009-10-202018-04-24Nyxoah SAAcred implant unit for modulation of nerves
US10751537B2 (en)2009-10-202020-08-25Nyxoah SAArced implant unit for modulation of nerves
US8585617B2 (en)2009-12-212013-11-19Nyxoah SADiagnosis and prediction of obstructive sleep apnea
WO2011059531A1 (en)2009-11-102011-05-19Imthera Medical, Inc.System for stimulating a hypoglossal nerve for controlling the position of a patient's tongue
US9833621B2 (en)2011-09-232017-12-05Setpoint Medical CorporationModulation of sirtuins by vagus nerve stimulation
WO2014169145A1 (en)2013-04-102014-10-16Setpoint Medical CorporationClosed-loop vagus nerve stimulation
EP2515996B1 (en)2009-12-232019-09-18Setpoint Medical CorporationNeural stimulation devices and systems for treatment of chronic inflammation
US8801728B2 (en)2010-01-292014-08-12Medtronic, Inc.Introduction of medical lead into patient
US8554339B2 (en)2010-01-292013-10-08Medtronic, Inc.Anchor assembly for use in occipital nerve stimulation
US9724126B2 (en)2010-01-292017-08-08Medtronic, Inc.Introduction of medical lead into patient
US8744098B2 (en)*2010-02-042014-06-03Apple Inc.Using an audio cable as an inductive charging coil
US11717681B2 (en)2010-03-052023-08-08Endostim, Inc.Systems and methods for treating gastroesophageal reflux disease
WO2011109739A1 (en)2010-03-052011-09-09Endostim, Inc.Device and implantation system for electrical stimulation of biological systems
US8831729B2 (en)2011-03-042014-09-09Endostim, Inc.Systems and methods for treating gastroesophageal reflux disease
US9950159B2 (en)2013-10-232018-04-24Mainstay Medical LimitedSystems and methods for restoring muscle function to the lumbar spine and kits for implanting the same
CA2792529C (en)2010-03-112018-06-05Mainstay Medical, Inc.Modular stimulator for treatment of back pain, implantable rf ablation system and methods of use
US9999763B2 (en)2012-06-132018-06-19Mainstay Medical LimitedApparatus and methods for anchoring electrode leads adjacent to nervous tissue
US11684774B2 (en)2010-03-112023-06-27Mainstay Medical LimitedElectrical stimulator for treatment of back pain and methods of use
US12097365B2 (en)2010-03-112024-09-24Mainstay Medical LimitedElectrical stimulator for the treatment of back pain and methods of use
US11786725B2 (en)2012-06-132023-10-17Mainstay Medical LimitedSystems and methods for restoring muscle function to the lumbar spine and kits for implanting the same
US9888864B2 (en)2010-03-122018-02-13Inspire Medical Systems, Inc.Method and system for identifying a location for nerve stimulation
US8918187B2 (en)*2010-03-312014-12-23Medtronic, IncMedical leads and related systems that include coiled filars with longitudinally straight ends
US8478425B2 (en)2010-03-312013-07-02Medtronic, Inc.Medical leads and related systems that include a lumen body that is joined to a lead body and that has multiple filar lumens
BR112012028015A2 (en)2010-05-022017-03-28Lake Biosciences Llc apparatus and method
US9272157B2 (en)2010-05-022016-03-01Nervive, Inc.Modulating function of neural structures near the ear
EP3002037B1 (en)2010-09-152018-06-06Cardiac Pacemakers, Inc.Automatic selection of lead configuration for a neural stimulation lead
US8983572B2 (en)2010-10-292015-03-17Inspire Medical Systems, Inc.System and method for patient selection in treating sleep disordered breathing
US9457186B2 (en)2010-11-152016-10-04Bluewind Medical Ltd.Bilateral feedback
US20120123498A1 (en)*2010-11-152012-05-17Rainbow Medical Ltd.Sleep apnea treatment system
US9186504B2 (en)2010-11-152015-11-17Rainbow Medical LtdSleep apnea treatment
RU2013127313A (en)2010-11-162014-12-27Те Борд Оф Трастиз Оф Те Лилэнд Стэнфорд Джуниор Юниверсити SYSTEMS AND METHODS FOR TREATING A DRY EYE
US9821159B2 (en)2010-11-162017-11-21The Board Of Trustees Of The Leland Stanford Junior UniversityStimulation devices and methods
BR112013013448A2 (en)*2010-11-302016-10-18Fabian Hermann Urban Füglister helical inserter
US9968775B2 (en)*2010-12-092018-05-15Medtronic, Inc.Method and apparatus for replacing lead extension without tunneling
US8783250B2 (en)2011-02-272014-07-22Covidien LpMethods and systems for transitory ventilation support
US9084859B2 (en)2011-03-142015-07-21Sleepnea LlcEnergy-harvesting respiratory method and device
US8714154B2 (en)2011-03-302014-05-06Covidien LpSystems and methods for automatic adjustment of ventilator settings
US8965499B2 (en)2011-04-292015-02-24Cyberonics, Inc.Overwrap for nerve stimulation system
US8986382B2 (en)*2011-05-032015-03-24Boston Scientific Neuromodulation CorporationTissue fixation and repair systems and methods
WO2012154865A2 (en)2011-05-092012-11-15Setpoint Medical CorporationSingle-pulse activation of the cholinergic anti-inflammatory pathway to treat chronic inflammation
US12172017B2 (en)2011-05-092024-12-24Setpoint Medical CorporationVagus nerve stimulation to treat neurodegenerative disorders
US11413458B2 (en)2011-05-192022-08-16Neuros Medical, Inc.Nerve cuff electrode for neuromodulation in large human nerve trunks
US10758723B2 (en)2011-05-192020-09-01Neuros Medical, Inc.Nerve cuff electrode for neuromodulation in large human nerve trunks
US8996114B2 (en)2011-06-282015-03-31Cardiac Pacemakers, Inc.Strain relief feature for an implantable medical device lead
EP2729213B1 (en)2011-07-072019-05-01Cardiac Pacemakers, Inc.Insulation and stability features for an implantable medical device lead
CA2843767C (en)*2011-08-022019-07-09Mainstay Medical LimitedApparatus for anchoring electrode leads for use with implantable neuromuscular electrical stimulator
JP6092212B2 (en)2011-08-112017-03-08インスパイア・メディカル・システムズ・インコーポレイテッドInspire Medical Systems, Inc. System for selecting a stimulation protocol based on detection results of respiratory effort
US20140249646A1 (en)*2011-08-292014-09-04Neurodan A/SSystem for recording electroneurographic activity
US8934992B2 (en)2011-09-012015-01-13Inspire Medical Systems, Inc.Nerve cuff
US9925367B2 (en)2011-09-022018-03-27Endostim, Inc.Laparoscopic lead implantation method
EP2564895B1 (en)*2011-09-052015-11-18Venus Concept LtdAn improved esthetic device for beautifying skin
US8983611B2 (en)2011-09-272015-03-17Cardiac Pacemakers, Inc.Neural control of central sleep apnea
CA2850315A1 (en)*2011-09-302013-04-04Nyxoah SADevice and method for modulating nerves using parallel electric fields
US8751017B2 (en)2011-12-122014-06-10Neurostream Technologies G.P.Reinforced, compliant electrode assembly
JP5694139B2 (en)*2011-12-282015-04-01日本光電工業株式会社 Device for detecting apnea / hypopnea during sleep
DE102012201073B4 (en)*2012-01-252014-05-08Dualis Medtech Gmbh Carrying device for carrying a transmitting coil on the body of a patient
WO2013111137A2 (en)2012-01-262013-08-01Rainbow Medical Ltd.Wireless neurqstimulatqrs
WO2013142053A1 (en)2012-03-212013-09-26Cardiac Pacemakers, Inc.Systems and methods for stimulation of vagus nerve
US9572983B2 (en)2012-03-262017-02-21Setpoint Medical CorporationDevices and methods for modulation of bone erosion
CN104582787A (en)*2012-04-022015-04-29生物控制医疗(Bcm)有限公司Electrode cuffs
US20130267837A1 (en)*2012-04-102013-10-10NeuroAccess TechnologiesElectrical lead positioning systems and methods
JP5875926B2 (en)*2012-04-112016-03-02オリンパス株式会社 Medical lead
US8849421B2 (en)*2012-04-192014-09-30Medtronic, Inc.Medical leads having forced strain relief loops
US9681836B2 (en)2012-04-232017-06-20Cyberonics, Inc.Methods, systems and apparatuses for detecting seizure and non-seizure states
AT512534B1 (en)*2012-04-262013-09-15Univ Wien Med Nerve cuff electrode assembly
US9308370B2 (en)2012-05-152016-04-12Imthera Medical, Inc.Stimulation of a hypoglossal nerve for controlling the position of a patient's tongue
US9186501B2 (en)2012-06-132015-11-17Mainstay Medical LimitedSystems and methods for implanting electrode leads for use with implantable neuromuscular electrical stimulator
US10327810B2 (en)2016-07-052019-06-25Mainstay Medical LimitedSystems and methods for enhanced implantation of electrode leads between tissue layers
US10195419B2 (en)2012-06-132019-02-05Mainstay Medical LimitedElectrode leads for use with implantable neuromuscular electrical stimulator
CA2877049C (en)*2012-06-212022-08-16Simon Fraser UniversityTransvascular diaphragm pacing systems and methods of use
US10362967B2 (en)2012-07-092019-07-30Covidien LpSystems and methods for missed breath detection and indication
US9504828B2 (en)*2012-07-262016-11-29Nyxoah SAElectrical contacts on a medical device patch
EP3300766B1 (en)*2012-07-262019-04-24Nyxoah SAImplant encapsulation
US11253712B2 (en)2012-07-262022-02-22Nyxoah SASleep disordered breathing treatment apparatus
US9907967B2 (en)2012-07-262018-03-06Adi MashiachTranscutaneous power conveyance device
US10052097B2 (en)2012-07-262018-08-21Nyxoah SAImplant unit delivery tool
JP2015529495A (en)*2012-08-032015-10-08コーニンクレッカ フィリップス エヌ ヴェ Apparatus and method for assisting subject's airway
EP2882336B1 (en)2012-08-092019-06-26University of Iowa Research FoundationCatheter systems for puncturing through a tissue structure
EP2888000A4 (en)2012-08-232016-07-06Endostim IncDevice and implantation system for electrical stimulation of biological systems
US8812125B2 (en)2012-08-312014-08-19Greatbatch Ltd.Systems and methods for the identification and association of medical devices
US9615788B2 (en)2012-08-312017-04-11Nuvectra CorporationMethod and system of producing 2D representations of 3D pain and stimulation maps and implant models on a clinician programmer
US8903496B2 (en)2012-08-312014-12-02Greatbatch Ltd.Clinician programming system and method
US9594877B2 (en)2012-08-312017-03-14Nuvectra CorporationVirtual reality representation of medical devices
US8761897B2 (en)2012-08-312014-06-24Greatbatch Ltd.Method and system of graphical representation of lead connector block and implantable pulse generators on a clinician programmer
US9507912B2 (en)2012-08-312016-11-29Nuvectra CorporationMethod and system of simulating a pulse generator on a clinician programmer
US10668276B2 (en)2012-08-312020-06-02Cirtec Medical Corp.Method and system of bracketing stimulation parameters on clinician programmers
US9180302B2 (en)2012-08-312015-11-10Greatbatch Ltd.Touch screen finger position indicator for a spinal cord stimulation programming device
US9259577B2 (en)2012-08-312016-02-16Greatbatch Ltd.Method and system of quick neurostimulation electrode configuration and positioning
EP2890416A4 (en)2012-08-312016-07-20Univ Florida MANAGEMENT OF COUGH AND DEGLUTITION
US9471753B2 (en)2012-08-312016-10-18Nuvectra CorporationProgramming and virtual reality representation of stimulation parameter Groups
US8868199B2 (en)2012-08-312014-10-21Greatbatch Ltd.System and method of compressing medical maps for pulse generator or database storage
US9042992B2 (en)2012-08-312015-05-26University Of Florida Research Foundation, Inc.Protecting airways
US8983616B2 (en)2012-09-052015-03-17Greatbatch Ltd.Method and system for associating patient records with pulse generators
US9375582B2 (en)2012-08-312016-06-28Nuvectra CorporationTouch screen safety controls for clinician programmer
US8757485B2 (en)2012-09-052014-06-24Greatbatch Ltd.System and method for using clinician programmer and clinician programming data for inventory and manufacturing prediction and control
US9767255B2 (en)2012-09-052017-09-19Nuvectra CorporationPredefined input for clinician programmer data entry
WO2014055393A1 (en)2012-10-022014-04-10Cardiac Pacemakers, Inc.Pinch to open cuff electrode
US9114250B2 (en)2012-10-022015-08-25Cardiac Pacemakers, Inc.Pinch to open cuff electrode
US9265458B2 (en)2012-12-042016-02-23Sync-Think, Inc.Application of smooth pursuit cognitive testing paradigms to clinical drug development
US9861812B2 (en)2012-12-062018-01-09Blue Wind Medical Ltd.Delivery of implantable neurostimulators
WO2014097055A1 (en)*2012-12-172014-06-26Koninklijke Philips N.V.Multi function docking module for a pressure support therapy system
JP6026674B2 (en)2012-12-282016-11-16カーディアック ペースメイカーズ, インコーポレイテッド Stimulation cuff and implantable device
EP2956208B1 (en)2013-02-132021-01-13Cardiac Pacemakers, Inc.Cuff electrode with integrated tendril
US20150297885A1 (en)*2013-02-262015-10-22Endostim, Inc.Implantable Electrical Stimulation Leads
US10004904B2 (en)2013-03-072018-06-26Imthera Medical, IncLead splitter for neurostimulation systems
US9265956B2 (en)2013-03-082016-02-23Oculeve, Inc.Devices and methods for treating dry eye in animals
US9380976B2 (en)2013-03-112016-07-05Sync-Think, Inc.Optical neuroinformatics
WO2014165124A1 (en)2013-03-122014-10-09Oculeve, Inc.Implant delivery devices, systems, and methods
US9072898B2 (en)2013-03-142015-07-07CyMedica, Inc.System and methods for treating or supporting human joints or a portion of the human body
US8870798B2 (en)*2013-03-142014-10-28CyMedica, Inc.Systems and methods for treating human joints
CN108744272A (en)2013-04-192018-11-06奥库利维公司Nose stimulating apparatus and method
US10065047B2 (en)2013-05-202018-09-04Nervive, Inc.Coordinating emergency treatment of cardiac dysfunction and non-cardiac neural dysfunction
EP3010583B1 (en)2013-06-172020-08-05Nyxoah SADynamic modification of modulation throughout a therapy period
US9539422B2 (en)2013-07-022017-01-10Greatbatch Ltd.Neurostimulator interconnection apparatus, system, and method
TWI617330B (en)*2013-08-062018-03-11Univ Chang Gung Negative pressure breathing muscle training system and method
TWI615168B (en)*2013-08-062018-02-21Univ Chang Gung Electric stimulation system and method for strengthening squat muscle group
CN105492067B (en)2013-08-272017-07-25哈洛纽罗公司Electrode system for electro photoluminescence
EP3038700B1 (en)2013-08-272020-03-11Halo Neuro, Inc.Method and system for providing electrical stimulation to a user
US9782585B2 (en)2013-08-272017-10-10Halo Neuro, Inc.Method and system for providing electrical stimulation to a user
US9827425B2 (en)2013-09-032017-11-28Endostim, Inc.Methods and systems of electrode polarity switching in electrical stimulation therapy
US11045293B2 (en)2013-10-282021-06-293Shape A/SMethod for applying design guides
EP3071288B1 (en)2013-11-192018-11-14The Cleveland Clinic FoundationSystem for treating obstructive sleep apnea using a neuromuscular stimulator
EP3091921B1 (en)2014-01-062019-06-19Farapulse, Inc.Apparatus for renal denervation ablation
EP3104768B1 (en)2014-02-112023-07-26Cyberonics, Inc.Systems for detecting and treating obstructive sleep apnea
EP2905006B8 (en)*2014-02-112017-06-07Sorin CRM SASDevice for discriminating the stages of sleep of a patient
EP2904969B1 (en)*2014-02-112022-01-05Sorin CRM SASDevice for treating the sleep apnea syndrome in a patient by kinaesthetic stimulation
WO2015123525A2 (en)2014-02-142015-08-20O'day John MNasopharyngeal device for obstructive sleep apnea syndrome
US10307086B2 (en)*2014-02-172019-06-04Hong Kong Baptist UniversityGait measurement with 3-axes accelerometer/gyro in mobile devices
CN111298285A (en)2014-02-252020-06-19奥库利维公司Polymer formulations for nasolacrimal stimulation
US20150283382A1 (en)*2014-04-042015-10-08Med-El Elektromedizinische Geraete GmbhRespiration Sensors For Recording Of Triggered Respiratory Signals In Neurostimulators
US20150283381A1 (en)2014-04-042015-10-08Med-El Elektromedizinische Geraete GmbhAcceleration Sensors For Recording Of Triggered Respiratory Signals In Neurostimulators
AU2015253735B2 (en)*2014-04-282018-03-01Med-El Elektromedizinische Geraete GmbhRespiration sensors for recording of triggered respiratory signals in neurostimulators
EP4238521A3 (en)*2014-05-072023-11-29Farapulse, Inc.Methods and apparatus for selective tissue ablation
WO2015175944A1 (en)2014-05-162015-11-19Gary LongMethods and apparatus for multi-catheter tissue ablation
US11246743B2 (en)*2014-06-042022-02-15Archis Health InvestmentsSystem and method for sensor driven intelligent oral appliance
WO2015192027A1 (en)2014-06-122015-12-17Iowa Approach Inc.Method and apparatus for rapid and selective transurethral tissue ablation
EP3154464B1 (en)2014-06-122025-03-12Boston Scientific Scimed, Inc.Apparatus for rapid and selective tissue ablation with cooling
EP4406589A3 (en)2014-07-222024-08-07Imthera Medical, Inc.Method for adjusting a system for stimulating a hypoglossal nerve
ES2792856T3 (en)2014-07-252020-11-12Oculeve Inc Stimulation patterns to treat dry eyes
US9808591B2 (en)2014-08-152017-11-07Covidien LpMethods and systems for breath delivery synchronization
EP3180069B1 (en)*2014-08-172020-05-13Nine Continents Medical, Inc.Miniature implatable neurostimulator system for sciatic nerves and their branches
CN107073263B (en)*2014-09-122021-07-23纽若斯医疗公司 Neural envelope electrodes for neuromodulation in large human neural trunks
DE102014014927A1 (en)*2014-10-072016-04-07Neuroloop GmbH Implantable electrode arrangement
EP3206613B1 (en)2014-10-142019-07-03Farapulse, Inc.Apparatus for rapid and safe pulmonary vein cardiac ablation
US10471268B2 (en)2014-10-162019-11-12Mainstay Medical LimitedSystems and methods for monitoring muscle rehabilitation
EP3209371A4 (en)2014-10-222018-10-24Oculeve, Inc.Implantable nasal stimulator systems and methods
AU2015335772B2 (en)2014-10-222020-07-09Oculeve, Inc.Contact lens for increasing tear production
CA2965186A1 (en)2014-10-222016-04-28Oculeve, Inc.Stimulation devices and methods for treating dry eye
US11311725B2 (en)2014-10-242022-04-26Setpoint Medical CorporationSystems and methods for stimulating and/or monitoring loci in the brain to treat inflammation and to enhance vagus nerve stimulation
US9950129B2 (en)2014-10-272018-04-24Covidien LpVentilation triggering using change-point detection
EP3220999A2 (en)2014-11-172017-09-27Endostim, Inc.Implantable electro-medical device programmable for improved operational life
JP6289666B2 (en)*2014-11-192018-03-07シャープ株式会社 Photodynamic therapy device
FR3028745B1 (en)*2014-11-242021-07-23Inst Nat Sante Rech Med VIBROTACTILE STIMULATION DEVICE
CN114209979A (en)*2014-11-262022-03-22Spr治疗股份有限公司Electrical stimulator for peripheral stimulation
GB201421448D0 (en)2014-12-032015-01-14Armighorn Medical LtdOral muscle training
EP3031491B1 (en)*2014-12-082019-01-30Sorin CRM SASSystem for treating a respiratory condition by kinesthetic stimulation, with selection of stimulation strategies
EP3031437B1 (en)*2014-12-082017-09-13Sorin CRM SASDevice for optimising treatment of sleep apnoea syndrome by kinesthetic stimulation
EP3031492B1 (en)*2014-12-082017-10-25Sorin CRM SASSystem for treating a respiratory condition by kinesthetic stimulation, with stabilisation control of the stimulation
US9764146B2 (en)2015-01-212017-09-19Bluewind Medical Ltd.Extracorporeal implant controllers
US10004896B2 (en)2015-01-212018-06-26Bluewind Medical Ltd.Anchors and implant devices
US9597521B2 (en)2015-01-212017-03-21Bluewind Medical Ltd.Transmitting coils for neurostimulation
US11406833B2 (en)2015-02-032022-08-09Setpoint Medical CorporationApparatus and method for reminding, prompting, or alerting a patient with an implanted stimulator
US10946195B2 (en)*2015-03-132021-03-16Case Western Reserve UniversitySystem and method for ensuring airway patency when asleep
AU2016233377B2 (en)2015-03-192020-04-30Inspire Medical Systems, Inc.Stimulation for treating sleep disordered breathing
US9935501B2 (en)*2015-04-102018-04-03Samsung Electro-Mechanics Co., Ltd.Wireless power transmitting and receiving device, apparatus including the same, and method
US20160354603A1 (en)*2015-06-052016-12-08The Alfred E. Mann Foundation For Scientific ResearchUpper airway stimulator systems for obstructive sleep apnea
US9782589B2 (en)2015-06-102017-10-10Bluewind Medical Ltd.Implantable electrostimulator for improving blood flow
CN108290037B (en)2015-10-262021-10-08福禄神经学公司Electrode positioning system and method
US10105540B2 (en)2015-11-092018-10-23Bluewind Medical Ltd.Optimization of application of current
US9713707B2 (en)2015-11-122017-07-25Bluewind Medical Ltd.Inhibition of implant migration
EP4252833A3 (en)2015-11-172023-11-15Inspire Medical Systems, Inc.Microstimulation sleep disordered breathing (sdb) therapy device
JP2018535077A (en)*2015-11-232018-11-29ザ ジェネラル ホスピタル コーポレイション System and method for percutaneous vagus nerve stimulation placed in the ear
CA3005969A1 (en)*2015-11-242017-06-01The Charles Stark Draper Laboratory, Inc.Laser-assisted drug delivery system
US10426958B2 (en)2015-12-042019-10-01Oculeve, Inc.Intranasal stimulation for enhanced release of ocular mucins and other tear proteins
US10493224B2 (en)2015-12-312019-12-03At&T Intellectual Property I, L.P.Apparatus and method for improving an artificial respirator
US20170189097A1 (en)2016-01-052017-07-06Iowa Approach Inc.Systems, apparatuses and methods for delivery of ablative energy to tissue
US10172673B2 (en)2016-01-052019-01-08Farapulse, Inc.Systems devices, and methods for delivery of pulsed electric field ablative energy to endocardial tissue
US10660702B2 (en)2016-01-052020-05-26Farapulse, Inc.Systems, devices, and methods for focal ablation
US10512505B2 (en)2018-05-072019-12-24Farapulse, Inc.Systems, apparatuses and methods for delivery of ablative energy to tissue
US12144541B2 (en)2016-01-052024-11-19Boston Scientific Scimed, Inc.Systems, apparatuses and methods for delivery of ablative energy to tissue
US10130423B1 (en)2017-07-062018-11-20Farapulse, Inc.Systems, devices, and methods for focal ablation
US10596367B2 (en)2016-01-132020-03-24Setpoint Medical CorporationSystems and methods for establishing a nerve block
US11471681B2 (en)2016-01-202022-10-18Setpoint Medical CorporationBatteryless implantable microstimulators
CN114904142A (en)2016-01-202022-08-16赛博恩特医疗器械公司Control of vagal nerve stimulation
EP3405255A4 (en)2016-01-202019-10-16Setpoint Medical Corporation IMPLANTABLE MICROSTIMULATORS AND INDUCTION RECHARGE SYSTEMS
US10583304B2 (en)2016-01-252020-03-10Setpoint Medical CorporationImplantable neurostimulator having power control and thermal regulation and methods of use
US10814127B2 (en)2016-02-052020-10-27Boston Scientific Neuromodulation CorporationSlotted sleeve neurostimulation device
WO2017139243A1 (en)2016-02-082017-08-17Halo Neuro, Inc.Method and system for improving provision of electrical stimulation
US10485969B2 (en)2016-02-192019-11-26Boston Scientific Neuromodulation CorporationElectrical stimulation cuff devices and systems
US10252048B2 (en)2016-02-192019-04-09Oculeve, Inc.Nasal stimulation for rhinitis, nasal congestion, and ocular allergies
DE102016103597A1 (en)*2016-02-292017-08-31Albert-Ludwigs-Universität Freiburg Implantable cuff electrode
WO2017192572A1 (en)2016-05-022017-11-09Oculeve, Inc.Intranasal stimulation for treatment of meibomian gland disease and blepharitis
US10493269B2 (en)2016-06-022019-12-03Boston Scientific Neuromodulation CorporationLeads for electrostimulation of peripheral nerves and other targets
WO2017218734A1 (en)2016-06-162017-12-21Iowa Approach, Inc.Systems, apparatuses, and methods for guide wire delivery
US10485443B2 (en)2016-06-202019-11-26Halo Neuro, Inc.Electrical interface system
US10709888B2 (en)2016-07-292020-07-14Boston Scientific Neuromodulation CorporationSystems and methods for making and using an electrical stimulation system for peripheral nerve stimulation
WO2018057745A1 (en)*2016-09-232018-03-29Kosmo Technologies, Inc.Methods and devices for positioning of a mandible of a subject for determining and manipulating an airway opening
WO2018063183A1 (en)*2016-09-282018-04-05Oday John MNasopharyngeal device for obstructive sleep apnea syndrome
US11819683B2 (en)2016-11-172023-11-21Endostim, Inc.Modular stimulation system for the treatment of gastrointestinal disorders
US10124178B2 (en)2016-11-232018-11-13Bluewind Medical Ltd.Implant and delivery tool therefor
US10905883B2 (en)2016-12-022021-02-02Boston Scientific Neuromodulation CorporationMethods and systems for selecting stimulation parameters for electrical stimulation devices
WO2018102535A1 (en)2016-12-022018-06-07Oculeve, Inc.Apparatus and method for dry eye forecast and treatment recommendation
US20180221660A1 (en)2017-02-012018-08-09The Alfred E. Mann Foundation For Scientific ResearchStimulator systems and methods for obstructive sleep apnea
KR102069613B1 (en)2017-02-212020-02-11에이피시스템 주식회사Apparatus for irradiating light
WO2018165481A1 (en)2017-03-082018-09-13Halo Neuro, Inc.System for electrical stimulation
EP3606603A1 (en)2017-04-062020-02-12Endostim, Inc.Implantable surface electrodes and method of implantation
US10617867B2 (en)2017-04-282020-04-14Farapulse, Inc.Systems, devices, and methods for delivery of pulsed electric field ablative energy to esophageal tissue
US20180318577A1 (en)2017-05-022018-11-08The Alfred E. Mann Foundation For Scientific ResearchNerve cuff electrode locking mechanism
US20180353764A1 (en)2017-06-132018-12-13Bluewind Medical Ltd.Antenna configuration
GB2563440B (en)*2017-06-162019-06-05Cardiaccs AsSecuring a sensor at the heart
EP3658223A1 (en)2017-07-282020-06-03Galvani Bioelectronics LimitedElectrode devices for neurostimulation
WO2019020983A1 (en)*2017-07-282019-01-31Galvani Bioelectronics LimitedElectrode devices for neurostimulation
EP3658222A1 (en)2017-07-282020-06-03Galvani Bioelectronics LimitedElectrode devices and methods of manufacturing
WO2019020985A1 (en)*2017-07-282019-01-31Galvani Bioelectronics LimitedElectrode devices for neurostimulation
WO2019032890A1 (en)2017-08-112019-02-14Inspire Medical Systems, Inc.Cuff electrode
WO2019036470A1 (en)2017-08-142019-02-21Setpoint Medical CorporationVagus nerve stimulation pre-screening test
US11291838B2 (en)2017-08-312022-04-05Mayo Foundation For Medical Education And ResearchSystems and methods for controlling breathing
EP3681391A1 (en)2017-09-122020-07-22Farapulse, Inc.Systems, apparatuses, and methods for ventricular focal ablation
US10507324B2 (en)2017-11-172019-12-17Halo Neuro, Inc.System and method for individualizing modulation
US11980720B2 (en)*2017-12-082024-05-14The Texas A&M University SystemWearable therapeutic intervention device for sleep disorders and methods of use thereof
CN111670061A (en)2017-12-132020-09-15纽若斯医疗公司Nerve cuff deployment device
WO2019140404A1 (en)*2018-01-142019-07-18Stimaire, Inc.Wireless neural stimulator with injectable
DE102018204036A1 (en)*2018-03-162019-09-19Neuroloop GmbH Implant in the form of a winding cuff electrode assembly
KR102505594B1 (en)2018-04-092023-03-06뉴로스 메디컬 인코포레이티드 Apparatus and method for setting capacitance
US20190336198A1 (en)2018-05-032019-11-07Farapulse, Inc.Systems, devices, and methods for ablation using surgical clamps
CN112118798B (en)2018-05-072024-09-20波士顿科学医学有限公司 Systems, devices and methods for filtering high voltage noise induced by pulsed electric field ablation
JP7399881B2 (en)2018-05-072023-12-18ファラパルス,インコーポレイテッド epicardial ablation catheter
CN112118884A (en)2018-05-142020-12-22柯惠有限合伙公司 System and method for respiratory effort detection with signal distortion
DE102018207709A1 (en)2018-05-172019-11-21Neuroloop GmbH Device for extravascular or extraneuronal attachment of a medical implant in the form of a winding cuff
CA3096130A1 (en)2018-06-012019-12-05Zennea Technologies Inc.Method and device for treating sleep related breathing disorders
TWI672118B (en)*2018-06-082019-09-21溫義輝Probe for nerve detection system
EP3603737B1 (en)2018-07-312020-08-26Flow Neuroscience ABPositioning of electrodes for transcranial brain stimulation
WO2020037145A1 (en)*2018-08-152020-02-20Cvrx, Inc.Devices and methods for percutaneous electrode implant
CN112955088B (en)2018-09-202024-11-26波士顿科学医学有限公司 Systems, devices and methods for delivering pulsed electric field ablation energy to endocardial tissue
US11097115B2 (en)*2018-09-242021-08-24Galvani Bioelectronics LimitedImplantable pulse generator with suture holes and methods for implanting the same
US20210402191A1 (en)*2018-09-242021-12-30Galvani Bioelectronics LimitedImplantable pulse generator with suture holes, methods for implanting the same, and encapsulation of external components in active implantable medical devices
US11260229B2 (en)2018-09-252022-03-01The Feinstein Institutes For Medical ResearchMethods and apparatuses for reducing bleeding via coordinated trigeminal and vagal nerve stimulation
WO2020070535A1 (en)*2018-10-032020-04-09Breas Medical AbDevices and methods for treating a breathing-related sleep disorder, methods of use and control processes for such a device
US11752287B2 (en)2018-10-032023-09-12Covidien LpSystems and methods for automatic cycling or cycling detection
GB2573028B (en)2018-10-172020-04-29Signifier Medical Tech LimitedOral muscle training
WO2020082127A1 (en)*2018-10-232020-04-30Saluda Medical Pty LimitedCharge monitor
EP3880104A4 (en)*2018-11-152022-07-27Centerline Biomedical, Inc.Systems and methods for registration using an anatomical measurement wire
FR3088554A1 (en)*2018-11-212020-05-22Sorin Crm Sas Implantable medical probe with strain relief device
FR3088553A1 (en)2018-11-212020-05-22Sorin Crm Sas Implantable lead
CN113905694B (en)*2019-01-252024-10-22维兰德·K·沙马Device for treating obstructive sleep apnea
WO2020179941A1 (en)*2019-03-052020-09-10서울대학교산학협력단Palatal implant and electrical stimulation system using same
US20200282215A1 (en)2019-03-062020-09-10Medtronic Xomed, LLCEvaluating stimulation eficacy for treating sleep apnea and lingual muscle tone sensing system for improved osa therapy
MX2021010788A (en)*2019-03-082022-01-18Univ VanderbiltSystems and methods for treating sleep disordered breathing.
US11478638B2 (en)*2019-03-222022-10-25Neurostim Technologies LlcDetection and treatment of obstructive sleep apnea
US11446485B2 (en)*2019-04-262022-09-20Nextern Innovation, LlcLead for the temporary stimulation of a peripheral nerve
ES2956271T3 (en)2019-05-022023-12-18Xii Medical Inc Implantable stimulation power receiver and systems
EP3989813A4 (en)*2019-06-282023-10-04ResMed Pty LtdBand with built-in stimulator
US12262988B2 (en)2019-07-252025-04-01Inspire Medical Systems, Inc.Respiration detection
JP7614171B2 (en)2019-07-252025-01-15インスパイア・メディカル・システムズ・インコーポレイテッド SYSTEMS AND METHODS FOR OPERATING AN IMPLANTABLE MEDICAL DEVICE BASED ON SENSE POSITION INFORMATION - Patent application
WO2021050829A1 (en)*2019-09-132021-03-18Vanderbilt UniversityNeuromodulation of the glossopharyngal nerve to improve sleep disordered breathing
US10625080B1 (en)2019-09-172020-04-21Farapulse, Inc.Systems, apparatuses, and methods for detecting ectopic electrocardiogram signals during pulsed electric field ablation
EP4045134A1 (en)2019-10-152022-08-24XII Medical, Inc.Biased neuromodulation lead and method of using same
EP3821940B1 (en)*2019-11-132025-01-01BIOTRONIK SE & Co. KGElectrode contact, electrode lead comprising an electrode contact and method for connecting an electrode contact to an electrical lead
US11065047B2 (en)2019-11-202021-07-20Farapulse, Inc.Systems, apparatuses, and methods for protecting electronic components from high power noise induced by high voltage pulses
US11497541B2 (en)2019-11-202022-11-15Boston Scientific Scimed, Inc.Systems, apparatuses, and methods for protecting electronic components from high power noise induced by high voltage pulses
US10842572B1 (en)2019-11-252020-11-24Farapulse, Inc.Methods, systems, and apparatuses for tracking ablation devices and generating lesion lines
JP7432736B2 (en)*2020-01-102024-02-16ニューエクセル2 エル.エル.シー. System and method for stimulating cranial nerves
US11666751B2 (en)2020-01-242023-06-06Medtronic Xomed, Inc.Combination obstructive sleep apnea trialing lead and chronic lead
US11273305B2 (en)2020-01-242022-03-15Medtronic Xomed, Inc.Medical lead for treating obstructive sleep apnea (OSA) with electrical stimulation
US11819233B2 (en)2020-01-242023-11-21Medtronic Xomed, Inc.Devices and techniques for separating tissue
US11426201B2 (en)2020-01-242022-08-30Medtronic Xomed, Inc.Treatment of obstructive sleep apnea (OSA)
US11198002B2 (en)2020-01-242021-12-14Medtronic Xomed, Inc.Needle and introducer used in lead placement for obstructive sleep apnea treatment
AU2021218682A1 (en)*2020-02-112022-08-25Stimaire, Inc.Less invasive and improved peripheral nerve stimulators for obstructive sleep apnea and other applications
AU2021219722A1 (en)2020-02-112022-09-08Neuros Medical, Inc.System and method for quantifying qualitative patient-reported data sets
EP4110454A4 (en)*2020-02-282024-03-20ResMed Pty LtdSystems and methods for aiding a user in breathing using implantable devices
WO2021236977A1 (en)2020-05-212021-11-25The Feinstein Institutes For Medical ResearchSystems and methods for vagus nerve stimulation
JP2023526870A (en)*2020-05-232023-06-23インスパイア・メディカル・システムズ・インコーポレイテッド Single or Multiple Nerve Stimulation to Treat Sleep Disordered Breathing
US11464985B2 (en)2020-05-262022-10-11Medtronic, Inc.Implantable medical device using internal sensors to determine when to switch operational modes
US12263336B2 (en)*2020-07-222025-04-01Nexalin Technology, Inc.Alternating current dynamic frequency stimulation system and method for opioid use disorder (OUD) and substance use disorder (SUD)
US12268437B2 (en)2020-07-242025-04-08Boston Scientific Scimed, Inc.Electric field application for single shot cardiac ablation by irreversible electroporation
AU2021336294A1 (en)2020-09-022023-03-30The Alfred E. Mann Foundation For Scientific ResearchElectrode leads having multi-application nerve cuffs and associated systems and methods
US20220134101A1 (en)*2020-10-302022-05-05Medtronic Xomed, Inc.Sleep apnea therapy
WO2022098786A1 (en)2020-11-042022-05-12Invicta Medical, Inc.Implantable electrodes with remote power delivery for treating sleep apnea, and associated systems and methods
WO2022125571A1 (en)*2020-12-082022-06-16The Regents Of The University Of CaliforniaBioelectric neuromodulation for hematopoiesis regulation during chemotherapy
US11691010B2 (en)2021-01-132023-07-04Xii Medical, Inc.Systems and methods for improving sleep disordered breathing
TWI820560B (en)2021-03-082023-11-01臺北醫學大學Manufacture method of dental appliance for treating obstructive sleep apnea-hypopnea syndrome
EP4313262B1 (en)2021-05-212025-04-02Boston Scientific Neuromodulation CorporationElectrical stimulation devices
US20220401746A1 (en)*2021-06-172022-12-22Bmseed LlcNovel peripheral nerve interface device
CA3224431A1 (en)*2021-06-292023-01-05Richard W. O'connorWearable devices for treating sleep apnea, and associated systems and methods
WO2023282922A1 (en)2021-07-092023-01-12The Alfred E. Mann Foundation For Scientific ResearchElectrode leads having multi-application helical nerve cuffs and associated systems and methods
US20250082927A1 (en)*2021-08-242025-03-13Cochlear LimitedWirelessly powered medical implant for treatment of sleep-disordered breathing
US11400299B1 (en)2021-09-142022-08-02Rainbow Medical Ltd.Flexible antenna for stimulator
WO2023230131A1 (en)*2022-05-242023-11-30Inspire Medical Systems, Inc.Sensing and applying stimulation in timed relationship
US11964154B1 (en)2022-12-222024-04-23Invicta Medical, Inc.Signal delivery devices to treat sleep apnea, and associated methods and systems
WO2024182674A1 (en)*2023-03-022024-09-06Xii Medical, Inc.Devices for treating sleep disordered breathing
US12246175B2 (en)2023-03-172025-03-11Invicta Medical, Inc.Methods for positioning signal delivery devices to treat sleep apnea, and associated devices and treatments
CN116473562A (en)*2023-06-212023-07-25博睿康科技(常州)股份有限公司Intelligent electrode and manufacturing method thereof
US20250032794A1 (en)*2023-07-242025-01-30The Alfred E. Mann Foundation For Scientific ResearchStimulation device and methods of stimulation
DE102023126302A1 (en)*2023-09-272025-03-27Neuroloop GmbH Medical implantable device
DE102023126630A1 (en)*2023-09-292025-04-03Neuroloop GmbH Medical implant

Citations (353)

* Cited by examiner, † Cited by third party
Publication numberPriority datePublication dateAssigneeTitle
US758030A (en)1903-06-301904-04-19Thomas CarenceNasal shield.
US1520930A (en)1923-09-011924-12-30Harry L CalhounFilter
US1701277A (en)1927-02-181929-02-05Willson Products IncValve device for respirators or the like
US1914418A (en)1930-02-151933-06-20Goyena Manuel GarciaNose protector
US2046664A (en)1935-11-071936-07-07Nasal Filter CoNasal filter
US2151227A (en)1937-02-121939-03-21Pawelek AnthonyNasal insert
US2237954A (en)1939-06-301941-04-08William R WilsonNasal filter and inhaler
US2243360A (en)1938-12-301941-05-27Slatis AbrahamFilter or medicament casing
US2274886A (en)1940-08-101942-03-03Harold D CarrollNasal respirator
US2526586A (en)1949-09-201950-10-17Leonard M ShuffNasal filter
US2693799A (en)1950-03-161954-11-09Jr Harry H HermanBreathing attachment for swimmers
US2777442A (en)1955-04-111957-01-15Zelano JosephNasal filter
US2928388A (en)1957-04-241960-03-15Alfred P JaroslawDisposable respirators
US3457917A (en)1966-02-171969-07-29John A MercurioNasal filtering device
US3513839A (en)1968-01-021970-05-26Matthew VacanteValved nose filter
US3680555A (en)1969-03-201972-08-01Draegerwerk AgProtective mask with annular flushing chamber
US3722509A (en)1971-01-051973-03-27J NebelNasal filters
US3774618A (en)1972-07-031973-11-27Avery Labor IncImplantable nerve stimulation electrode
US3865106A (en)1974-03-181975-02-11Bernard P PalushPositive pressure breathing circuit
US3884223A (en)1974-06-261975-05-20Lawrence Peska Ass IncNasal filter
US3893463A (en)1973-12-071975-07-08Medtronic IncDual channel stimulator
US3906936A (en)1974-02-151975-09-23Mutaz B HabalNasal air flow detection method for speech evaluation
JPS53118893A (en)1977-03-281978-10-17Univ Case Western ReserveContinuous proper air path pressure feeder
US4160255A (en)1976-10-041979-07-03Mitogiken, Ltd.Recording apparatus with intermittent power usage
US4160252A (en)1977-03-251979-07-03U.S. Philips CorporationMethod of determining the direction of a radio source and radio interferometer system
US4178524A (en)1976-09-011979-12-11Ritter James CRadioisotope photoelectric generator
US4200440A (en)1979-02-211980-04-29The Air Preheater Company, Inc.Filter construction
US4220150A (en)1978-09-131980-09-02King John RNasal dust filter
US4221217A (en)1978-05-011980-09-09Amezcua Saul ONasal device
US4225034A (en)1978-07-031980-09-30The Sardee CorporationContainer conveying and elevating apparatus
US4239918A (en)1978-12-061980-12-16General Electric CompanyMeta, para-substituted isopropylidene bisphenols and methods for making
US4242987A (en)1977-07-121981-01-06Hans ViessmannConnecting arrangement for a heating boiler
US4267831A (en)1979-09-241981-05-19Aguilar Rogelio MNasal air filter and medicament dispenser device
US4283867A (en)1979-12-051981-08-18Roscoe Brown CorporationBackfilling apparatus with adjustable filling augers
US4302951A (en)1979-12-261981-12-01Borg-Warner CorporationTorsional vibration damper
US4313442A (en)1980-07-211982-02-02Cardiac Pacemakers, Inc.Atrial rate sensitive cardiac pacer apparatus
US4346398A (en)1980-10-271982-08-24Zenith Radio CorporationAutomatic clock phase selector
US4374527A (en)1978-07-191983-02-22Medtronic, Inc.Body stimulation lead
US4414986A (en)1982-01-291983-11-15Medtronic, Inc.Biomedical stimulation lead
US4506666A (en)1982-12-031985-03-26Kircaldie, Randall And McnabMethod and apparatus for rectifying obstructive apnea
US4567892A (en)1982-03-161986-02-04Gianni PlicchiImplantable cardiac pacemaker
US4573481A (en)1984-06-251986-03-04Huntington Institute Of Applied ResearchImplantable electrode array
US4602624A (en)1984-10-111986-07-29Case Western Reserve UniversityImplantable cuff, method of manufacture, and method of installation
US4612934A (en)1981-06-301986-09-23Borkan William NNon-invasive multiprogrammable tissue stimulator
US4777963A (en)1987-06-181988-10-18Mckenna KevinRespiration monitor
US4830008A (en)1987-04-241989-05-16Meer Jeffrey AMethod and system for treatment of sleep apnea
US4899750A (en)1988-04-191990-02-13Siemens-Pacesetter, Inc.Lead impedance scanning system for pacemakers
US4915105A (en)1988-10-281990-04-10Lee Tien ChuMiniature respiratory apparatus
US4919136A (en)1987-09-281990-04-24Eckhard AltVentilation controlled rate responsive cardiac pacemaker
US4934368A (en)1988-01-211990-06-19Myo/Kinetics Systems, Inc.Multi-electrode neurological stimulation apparatus
US4940065A (en)1989-01-231990-07-10Regents Of The University Of CaliforniaSurgically implantable peripheral nerve electrode
US4960133A (en)1988-11-211990-10-02Brunswick Manufacturing Co., Inc.Esophageal electrode
US4979511A (en)1989-11-031990-12-25Cyberonics, Inc.Strain relief tether for implantable electrode
US4996983A (en)1989-01-311991-03-05Amrhein Floyd EInhaler filtration device with housing supportable by spectacle temple
US5016808A (en)1989-09-141991-05-21Cardiac Pacemakers, Inc.Implantable tapered spiral endocardial lead for use in internal defibrillation
US5036862A (en)1987-04-061991-08-06Cordis CorporationImplantable, self-retaining lead
US5095905A (en)1990-06-071992-03-17Medtronic, Inc.Implantable neural electrode
US5105826A (en)1990-10-261992-04-21Medtronic, Inc.Implantable defibrillation electrode and method of manufacture
US5121754A (en)1990-08-211992-06-16Medtronic, Inc.Lateral displacement percutaneously inserted epidural lead
US5133354A (en)1990-11-081992-07-28Medtronic, Inc.Method and apparatus for improving muscle tone
US5146918A (en)1991-03-191992-09-15Medtronic, Inc.Demand apnea control of central and obstructive sleep apnea
US5158080A (en)1990-11-081992-10-27Medtronic, Inc.Muscle tone
US5174287A (en)1991-05-281992-12-29Medtronic, Inc.Airway feedback measurement system responsive to detected inspiration and obstructive apnea event
US5178156A (en)1989-06-201993-01-12Chest CorporationApnea preventive stimulating device
US5190053A (en)1991-02-281993-03-02Jeffrey A. Meer, Revocable Living TrustMethod and apparatus for electrical sublingual stimulation
US5211173A (en)1991-01-091993-05-18Medtronic, Inc.Servo muscle control
US5215082A (en)1991-04-021993-06-01Medtronic, Inc.Implantable apnea generator with ramp on generator
US5281219A (en)1990-11-231994-01-25Medtronic, Inc.Multiple stimulation electrodes
US5300094A (en)1991-01-091994-04-05Medtronic, Inc.Servo muscle control
US5324321A (en)1992-12-221994-06-28Medtronic, Inc.Medical electrical lead having sigmoidal conductors and non-circular lumens
US5335657A (en)1991-05-031994-08-09Cyberonics, Inc.Therapeutic treatment of sleep disorder by nerve stimulation
US5344438A (en)1993-04-161994-09-06Medtronic, Inc.Cuff electrode
US5388578A (en)1992-01-141995-02-14Incontrol, Inc.Electrode system for use with an implantable cardiac patient monitor
US5392773A (en)1994-04-131995-02-28Bertrand; Archie A.Respiratory particulate filter
US5417205A (en)1994-06-071995-05-23Wang; Jen-YiAir filter for the nose
US5425359A (en)1994-08-291995-06-20Liou; Nan-TienNose plug structure with filter
US5458629A (en)1994-02-181995-10-17Medtronic, Inc.Implantable lead ring electrode and method of making
US5483969A (en)1994-09-211996-01-16Medtronic, Inc.Method and apparatus for providing a respiratory effort waveform for the treatment of obstructive sleep apnea
US5485836A (en)1987-03-201996-01-23Lincoln; Robert A.Nose worn air filter
US5485851A (en)1994-09-211996-01-23Medtronic, Inc.Method and apparatus for arousal detection
US5487756A (en)1994-12-231996-01-30Simon Fraser UniversityImplantable cuff having improved closure
US5511543A (en)1992-08-181996-04-30Shirley; Terry L.Disposable resuscitation device having unidirectional valve
US5522862A (en)1994-09-211996-06-04Medtronic, Inc.Method and apparatus for treating obstructive sleep apnea
US5522382A (en)1987-06-261996-06-04Rescare LimitedDevice and method for treating obstructed breathing having a delay/ramp feature
US5531778A (en)1994-09-201996-07-02Cyberonics, Inc.Circumneural electrode assembly
US5540731A (en)*1994-09-211996-07-30Medtronic, Inc.Method and apparatus for pressure detecting and treating obstructive airway disorders
US5540733A (en)1994-09-211996-07-30Medtronic, Inc.Method and apparatus for detecting and treating obstructive sleep apnea
US5540732A (en)1994-09-211996-07-30Medtronic, Inc.Method and apparatus for impedance detecting and treating obstructive airway disorders
US5540734A (en)1994-09-281996-07-30Zabara; JacobCranial nerve stimulation treatments using neurocybernetic prosthesis
US5546938A (en)1995-08-241996-08-20Mckenzie; Shirley T.ICU patients ventilator tube holding device
US5549655A (en)1994-09-211996-08-27Medtronic, Inc.Method and apparatus for synchronized treatment of obstructive sleep apnea
US5568808A (en)1995-08-081996-10-29Amtec Products, IncorporatedNose filters
US5591216A (en)1995-05-191997-01-07Medtronic, Inc.Method for treatment of sleep apnea by electrical stimulation
US5630411A (en)1993-01-121997-05-20Nellcor Puritan Bennett IncorporatedValve for use with inhalation/exhalation respiratory phase detection circuit
US5682881A (en)1996-10-211997-11-04Winthrop; NeilNasal CPAP/Cannula and securement apparatus
JPH09294819A (en)1996-05-021997-11-18孝明 ▲崎▼Nose mask
US5697105A (en)1996-09-041997-12-16White; MarkHunting mask
US5697363A (en)1996-04-121997-12-16Albert Einstein Healthcare NetworkInhalation and monitoring mask with headset
US5730122A (en)1996-11-121998-03-24Cprx, Inc.Heart failure mask and methods for increasing negative intrathoracic pressures
US5740798A (en)1994-04-221998-04-21Mckinney; Stella H.Disposable nasal band filter
US5752511A (en)1996-11-221998-05-19Simmons; Carl J.Universal medical tube retainer and nasal wall tissue dilator
US5787884A (en)1994-08-261998-08-04The University Of SydneyNasal and oral filters
US5848589A (en)1997-09-181998-12-15Welnetz; Robert J.Altitude mask simulator
US5855552A (en)1994-09-211999-01-05Ep Technologies, Inc.Catheter having ring electrodes secured thereon
US5871531A (en)1997-09-251999-02-16Medtronic, Inc.Medical electrical lead having tapered spiral fixation
US5890491A (en)1997-09-031999-04-06Amtec Products, Inc.Nose filter
US5895360A (en)1996-06-261999-04-20Medtronic, Inc.Gain control for a periodic signal and method regarding same
US5919220A (en)1994-09-161999-07-06Fraunhofer Gesellschaft Zur Foerderung Der Angewandten Forschung E.V.Cuff electrode
US5922014A (en)1997-09-021999-07-13Medtronic, Inc.Single pass lead and method of use
US5938596A (en)1997-03-171999-08-17Medtronic, Inc.Medical electrical lead
US5944680A (en)1996-06-261999-08-31Medtronic, Inc.Respiratory effort detection method and apparatus
US5947119A (en)1997-10-311999-09-07Reznick; Jerald M.Therapeutic process and apparatus for nasal passages
US6010459A (en)1996-04-092000-01-04Silkoff; Philip E.Method and apparatus for the measurement of components of exhaled breath in humans
US6015389A (en)1995-12-062000-01-18Btg International LimitedImpedance pneumography
US6021352A (en)1996-06-262000-02-01Medtronic, Inc,Diagnostic testing methods and apparatus for implantable therapy devices
US6041780A (en)1995-06-072000-03-28Richard; Ron F.Pressure control for constant minute volume
US6066165A (en)1998-04-302000-05-23Racz; Gabor BMedical lead with sigma feature
US6098624A (en)1996-12-162000-08-08Utamaru; MasanobuSimple mask for protection of respiratory system
US6119690A (en)1998-12-042000-09-19Pantaleo; Joseph M.Nostril filter system
US6126611A (en)1998-02-042000-10-03Medtronic, Inc.Apparatus for management of sleep apnea
US6132384A (en)1996-06-262000-10-17Medtronic, Inc.Sensor, method of sensor implant and system for treatment of respiratory disorders
US6198970B1 (en)1995-10-272001-03-06Esd Limited Liability CompanyMethod and apparatus for treating oropharyngeal respiratory and oral motor neuromuscular disorders with electrical stimulation
US6205360B1 (en)1995-09-072001-03-20Cochlear LimitedApparatus and method for automatically determining stimulation parameters
US6217527B1 (en)1998-09-302001-04-17Lumend, Inc.Methods and apparatus for crossing vascular occlusions
US6231546B1 (en)1998-01-132001-05-15Lumend, Inc.Methods and apparatus for crossing total occlusions in blood vessels
US6240316B1 (en)1998-08-142001-05-29Advanced Bionics CorporationImplantable microstimulation system for treatment of sleep apnea
US6244267B1 (en)1999-07-082001-06-12DRäGER MEDIZINTECHNICK GMBHRespirator with a pressure relief valve
US6251126B1 (en)1998-04-232001-06-26Medtronic IncMethod and apparatus for synchronized treatment of obstructive sleep apnea
US6269269B1 (en)1998-04-232001-07-31Medtronic Inc.Method and apparatus for synchronized treatment of obstructive sleep apnea
US6292703B1 (en)1998-10-082001-09-18Biotronik Mess-Und Therapiegerate Gmbh & Co.Neural electrode arrangement
US20010031929A1 (en)1999-12-282001-10-18O'toole JamesEnd tidal carbon dioxide sampling device
WO2002024279A1 (en)2000-09-212002-03-283M Innovative Properties CompanyRespirator that includes an integral filter element, an exhalation valve, and impactor element
US6366815B1 (en)1997-01-132002-04-02Neurodan A /SImplantable nerve stimulator electrode
US20020049479A1 (en)2000-10-202002-04-25Pitts Walter C.Method and apparatus for creating afferents to prevent obstructive sleep apnea
US20020092527A1 (en)2000-03-132002-07-18Wood Thomas J.Ventilation interface for sleep apnea therapy
US20020128700A1 (en)2001-03-082002-09-12Cross Thomas E.Lead with adjustable angular and spatial relationships between electrodes
US20020156507A1 (en)*2001-04-052002-10-24Werner LindenthalerPacemaker for bilateral vocal cord autoparalysis
US20020165462A1 (en)2000-12-292002-11-07Westbrook Philip R.Sleep apnea risk evaluation
US20020166556A1 (en)2001-05-092002-11-14Joseph JacobNose airflow enhancer and filter for airborne solids and pathogens
US6484725B1 (en)2001-06-252002-11-26Min Hung ChiNose plug device having air breathing structure
US20020195109A1 (en)2001-06-252002-12-263M Innovative Properties CompanyRespirator valve
US20020195108A1 (en)2001-06-252002-12-263M Innovative Properties CompanyRespirator valve
WO2003000133A1 (en)2001-06-262003-01-03C-Lect Medical LtdRespiration monitoring equipment
US20030034031A1 (en)2000-05-222003-02-20Sleep Up Ltd.Pacifier and method of use thereof
US20030040785A1 (en)2001-08-212003-02-27Maschino Steve E.Circumneural electrode assembly
US6542776B1 (en)1999-04-142003-04-01Transneuronix Inc.Gastric stimulator apparatus and method for installing
US20030078643A1 (en)2001-10-192003-04-24Schulman Joseph H.Electrically sensing and stimulating system for placement of a nerve stimulator or sensor
US20030083696A1 (en)1997-09-032003-05-01Hadasit Medical Research Service & Development CompanyPacifier
US6561188B1 (en)2000-08-212003-05-13Ellis Alan DNasal breathing apparatus and methods
US20030106556A1 (en)1999-12-102003-06-12Vladimir AlperovichRespiratory nasal filter
US20030106555A1 (en)2000-02-242003-06-12Euan ToveyNasal filter and sampler
US20030114905A1 (en)1999-10-012003-06-19Kuzma Janusz A.Implantable microdevice with extended lead and remote electrode
US6587725B1 (en)1998-07-272003-07-01Dominique DurandMethod and apparatus for closed-loop stimulation of the hypoglossal nerve in human patients to treat obstructive sleep apnea
US6606521B2 (en)2001-07-092003-08-12Neuropace, Inc.Implantable medical lead
US20030153953A1 (en)*2002-02-142003-08-14Euljoon ParkStimulation device for sleep apnea prevention, detection and treatment
US6609031B1 (en)1996-06-072003-08-19Advanced Neuromodulation Systems, Inc.Multiprogrammable tissue stimulator and method
US20030167018A1 (en)2002-03-042003-09-04Robert WyckoffSleep apnea device and method thereof
US6626179B1 (en)2000-09-292003-09-30Philip PedleyBreathing valve for improving oxygen absorption
WO2003082393A1 (en)2002-03-282003-10-09Optinose AsNasal devices
US20030195571A1 (en)2002-04-122003-10-16Burnes John E.Method and apparatus for the treatment of central sleep apnea using biventricular pacing
US6636767B1 (en)1999-09-292003-10-21Restore Medical, Inc.Implanatable stimulation device for snoring treatment
JP2003305135A (en)2002-04-172003-10-28Takao AkeuraBandage type nose mask
US6641542B2 (en)2001-04-302003-11-04Medtronic, Inc.Method and apparatus to detect and treat sleep respiratory events
US6647289B2 (en)1998-02-062003-11-11Intermedics Inc.Non-invasive cardiorespiratory monitor with synchronized bioimpedance sensing
US20030209145A1 (en)2002-02-142003-11-13Soper Adrian JohnFiltration device
US20030216789A1 (en)2002-05-142003-11-20The Foundry, Inc.Method and system for treating sleep apnea
US6651652B1 (en)1998-06-302003-11-25Siemens-Elema AbMethod for identifying respiration attempts by analyzing neuroelectrical signals, and respiration detector and respiratory aid system operating according to the method
US20040015204A1 (en)2002-06-202004-01-22Whitehurst Todd K.Implantable microstimulators and methods for unidirectional propagation of action potentials
US20040020489A1 (en)2002-07-252004-02-05Gail AlstonNasal mask with replaceable filter
US20040049241A1 (en)2002-09-102004-03-11Therapeutic Innovations, Inc.Distributed muscle stimulator
US20040055603A1 (en)2002-09-232004-03-25Bruce Carol Jean EmeryIntra-nasal filter device
US6718982B2 (en)2001-05-072004-04-13Mark A. SmithFace mask incorporating respiratory flow sensor
US6721603B2 (en)2002-01-252004-04-13Cyberonics, Inc.Nerve stimulation as a treatment for pain
US20040089303A1 (en)2002-11-112004-05-13Dennis ChienNose filter device
US20040111139A1 (en)2002-12-102004-06-10Mccreery Douglas B.Apparatus and methods for differential stimulation of nerve fibers
US20040116819A1 (en)2001-10-012004-06-17Eckhard AltCongestive heart failure monitor and ventilation measuring implant
US20040116978A1 (en)2002-12-062004-06-17Kerry BradleyMethod for determining stimulation parameters
US20040122497A1 (en)2002-12-192004-06-24Yongxing ZhangImplantable lead for septal placement of electrode with fixation mechanism in the pulmonary artery
US20040138581A1 (en)2002-10-152004-07-15Medtronic, Inc.Signal quality monitoring and control for a medical device system
US6772015B2 (en)2000-12-292004-08-03Medtronic, IncBifurcated lead system for a cardiac vein
US20040153127A1 (en)2003-01-152004-08-05Alfred E. Mann Institute For Biomedical Engineering At The University Of Southern CalifornTreatments for snoring using injectable neuromuscular stimulators
US20040162499A1 (en)2002-10-042004-08-19Fumiya NagaiAbnormal respiration detecting system and method for detecting the same
US6799575B1 (en)2001-04-212004-10-05Aaron CarterCannula for the separation of inhaled and exhaled gases
US20040194784A1 (en)2003-04-012004-10-07Archie BertrandRespiratory particulate filter
US20040215290A1 (en)*2001-06-212004-10-28Zealear David LMethod for promoting reinnervation of denervated tissue
US20040215288A1 (en)2003-04-252004-10-28Lee Michael T.Identifying combinations of electrodes for neurostimulation therapy
US6819958B2 (en)2001-02-202004-11-16Biophan Technologies, Inc.Electromagnetic interference immune tissue invasive system
US6829503B2 (en)2001-10-012004-12-07Scicotec GmbhCongestive heart failure monitor
US20040260310A1 (en)2002-10-232004-12-23Medtronic, Inc.Medical lead and method
US20040261791A1 (en)2003-06-242004-12-30Horian Richard C.Nasal dilator and method of nasal dilation
US20050004610A1 (en)2003-07-022005-01-06Jaeho KimCardiac cycle synchronized sampling of impedance signal
US20050010265A1 (en)2003-04-022005-01-13Neurostream Technologies Inc.Fully implantable nerve signal sensing and stimulation device and method for treating foot drop and other neurological disorders
WO2005004993A1 (en)2003-07-122005-01-20Lixin ZhouA nasal filter
US20050038490A1 (en)2001-08-312005-02-17Biocontrol Medical Ltd.Electrode assembly for nerve control
USRE38705E1 (en)1996-04-302005-02-22Medtronic, Inc.Method and device for electronically controlling the beating of a heart using venous electrical stimulation of nerve fibers
US20050043644A1 (en)2003-08-182005-02-24Stahmann Jeffrey E.Prediction of disordered breathing
US20050043772A1 (en)2003-08-182005-02-24Stahmann Jeffrey E.Therapy triggered by prediction of disordered breathing
US6876885B2 (en)2001-01-312005-04-05Medtronic, Inc.Implantable bifurcated gastrointestinal lead with active fixation
US20050076908A1 (en)2003-09-182005-04-14Kent LeeAutonomic arousal detection system and method
US6881192B1 (en)2002-06-122005-04-19Pacesetter, Inc.Measurement of sleep apnea duration and evaluation of response therapies using duration metrics
US20050085874A1 (en)2003-10-172005-04-21Ross DavisMethod and system for treating sleep apnea
US20050085866A1 (en)2003-10-152005-04-21Tehrani Amir J.Breathing disorder and precursor predictor and therapy delivery device and method
US6890306B2 (en)2001-12-142005-05-10Ela Medical S.A.Active medical device for the diagnosis of the sleep apnea syndrome
US20050098176A1 (en)2001-07-122005-05-12Helmut HoffrichterRespiratory therapy device for keeping free the natural respiratory tract of a human body and the use thereof in order to prevent the sound of snoring
US20050101833A1 (en)2003-09-022005-05-12Biotronik Gmbh & Co. KgApparatus for the treatment of sleep apnea
US20050119711A1 (en)2003-01-102005-06-02Cho Yong K.Apparatus and method for monitoring for disordered breathing
US6904320B2 (en)2002-02-142005-06-07Pacesetter, Inc.Sleep apnea therapy device using dynamic overdrive pacing
US20050165457A1 (en)2004-01-262005-07-28Michael BenserTiered therapy for respiratory oscillations characteristic of Cheyne-Stokes respiration
US20050209643A1 (en)2004-03-162005-09-22Heruth Kenneth TControlling therapy based on sleep quality
US20050209513A1 (en)2004-03-162005-09-22Heruth Kenneth TCollecting sleep quality information via a medical device
US20050234523A1 (en)2002-04-082005-10-20Levin Howard RRenal nerve stimulation method and apparatus for treatment of patients
US20050240241A1 (en)2003-06-092005-10-27Yun Anthony JTreatment of conditions through modulation of the autonomic nervous system
US20050251216A1 (en)1996-04-302005-11-10Medtronic, Inc.Method and device for electronically controlling the beating of a heart
US20050261747A1 (en)2003-05-162005-11-24Schuler Eleanor LMethod and system to control respiration by means of neuro-electrical coded signals
US20050267380A1 (en)2004-04-042005-12-01Ela Medical S.A.Active implantable medical device equipped with means for the diagnosis of respiratory disorders, with sophisticated detection of respiratory cycles with artifacts
US20050277999A1 (en)2004-06-102005-12-15Ndi Medical, LlcImplantable pulse generator for providing functional and/or therapeutic stimulation of muscles and /or nerves and/or central nervous system tissue
US6978171B2 (en)2002-03-152005-12-20Medtronic, Inc.Automated impedance measurement of an implantable medical device
US20060004429A1 (en)2004-02-122006-01-05Ndi Medical, Inc.Lead and electrode structures sized and configured for implantation in adipose tissue and associated methods of implantation
US20060005842A1 (en)2004-07-092006-01-12Rashad M ANasal pressure sensor oxygen therapy device
US20060025828A1 (en)2004-07-282006-02-02Armstrong Randolph KImpedance measurement for an implantable device
US20060030919A1 (en)2004-08-042006-02-09Ndi Medical, LlcDevices, systems, and methods employing a molded nerve cuff electrode
US20060032497A1 (en)2000-06-162006-02-16Rajiv DoshiMethods and devices for improving breathing in patients with pulmonary disease
US20060041295A1 (en)2004-08-172006-02-23Osypka Thomas PPositive fixation percutaneous epidural neurostimulation lead
US20060052836A1 (en)2004-09-082006-03-09Kim Daniel HNeurostimulation system
US20060058852A1 (en)2004-09-102006-03-16Steve KohMulti-variable feedback control of stimulation for inspiratory facilitation
US20060058588A1 (en)2004-09-022006-03-16Proteus Biomedical, Inc.Methods and apparatus for tissue activation and monitoring
US20060064029A1 (en)2002-07-032006-03-23Tel-Aviv University Future Technology Development L.P.Bio-impedance apparatus and method
US20060064138A1 (en)2004-04-302006-03-23Francisco VelascoMethod of treating mood disorders and/or anxiety disorders by brain stimulation
US7027869B2 (en)1998-01-072006-04-11Asthmatx, Inc.Method for treating an asthma attack
US20060079802A1 (en)2002-04-302006-04-13Medtronic, Inc.Method and apparatus to detect and monitor the frequency of obstructive sleep apnea
WO2006045251A1 (en)2004-10-292006-05-04Lam Philip Y TNose mask
US20060095088A1 (en)2004-10-212006-05-04Dirk De RidderNew stimulation design for neuromodulation
US20060111755A1 (en)2003-05-162006-05-25Stone Robert TMethod and system to control respiration by means of neuro-electrical coded signals
US7054692B1 (en)2001-06-222006-05-30Advanced Bionics CorporationFixation device for implantable microdevices
US20060116739A1 (en)2002-05-232006-06-01Nir BetserElectrode assembly for nerve control
US20060129189A1 (en)1998-01-152006-06-15Regenesis Biomedical, Inc.Pulsed electromagnetic energy treatment apparatus and method
WO2006063339A2 (en)2004-12-082006-06-15Ventus Medical, Inc.Respiratory devices and methods of use
US7065410B2 (en)2000-09-182006-06-20Cameron Health, Inc.Subcutaneous electrode with improved contact shape for transthorasic conduction
US20060135886A1 (en)2004-12-022006-06-22Biotronik Crm Patent AgDevice for determining thoracic impedance
US20060136024A1 (en)2004-12-222006-06-22Biocontrol Medical Ltd.Construction of electrode assembly for nerve control
US20060142815A1 (en)2003-10-152006-06-29Tehrani Amir JDevice and method for treating obstructive sleep apnea
US20060149345A1 (en)2003-09-122006-07-06Ndi Medical, LlcNeuromodulation stimulation for the restoration of sexual function
US20060149334A1 (en)*2003-10-152006-07-06Tehrani Amir JDevice and method for controlling breathing
US20060150980A1 (en)2003-07-022006-07-13Yung Ho KimAnion emission and anti-dust nose mask
US20060155341A1 (en)2003-10-152006-07-13Tehrani Amir JDevice and method for biasing lung volume
US7082331B1 (en)2004-04-212006-07-25Pacesetter, Inc.System and method for applying therapy during hyperpnea phase of periodic breathing using an implantable medical device
US20060167497A1 (en)2005-01-272006-07-27Cyberonics, Inc.Implantable medical device having multiple electrode/sensor capability and stimulation based on sensed intrinsic activity
US7087053B2 (en)2004-05-272006-08-08St. Jude Medical, Atrial Fibrillation Division, Inc.Catheter with bifurcated, collapsible tip for sensing and ablating
US20060184204A1 (en)2005-02-112006-08-17Advanced Bionics CorporationImplantable microstimulator having a separate battery unit and methods of use thereof
US7094206B2 (en)1999-04-232006-08-22The Trustees Of Tufts CollegeSystem for measuring respiratory function
US20060195170A1 (en)2002-05-232006-08-31Ehud CohenElectrode assembly for nerve control
US20060211951A1 (en)2002-05-292006-09-21Zoran MilijasevicImplantable bladder sensor
US7117036B2 (en)2002-06-272006-10-03Pacesetter, Inc.Using activity-based rest disturbance as a metric of sleep apnea
US20060224211A1 (en)2005-03-312006-10-05Durand Dominique MMethod of treating obstructive sleep apnea using electrical nerve stimulation
US20060241708A1 (en)2005-04-222006-10-26Willem BouteMultiple sensors for sleep apnea with probability indication for sleep diagnosis and means for automatic activation of alert or therapy
US20060241506A1 (en)2005-04-252006-10-26Melker Richard JMethod and apparatus for diagnosing respiratory disorders and determining the degree of exacerbations
US7128717B1 (en)2005-09-292006-10-31Washington UniversityMethod for determining airway obstruction
US20060247729A1 (en)2003-10-152006-11-02Tehrani Amir JMultimode device and method for controlling breathing
US20060259079A1 (en)2005-04-302006-11-16Medtronic, Inc.Impedance-based stimulation adjustment
US20060264777A1 (en)2005-04-292006-11-23Medtronic, Inc.Event-based lead impedance monitoring
US7142919B2 (en)2003-10-242006-11-28Medtronic, Inc.Reconfigurable, fault tolerant multiple-electrode cardiac lead systems
US20060271118A1 (en)2005-05-252006-11-30Cardiac Pacemakers, Inc.Implantable neural stimulator with mode switching
US20060266369A1 (en)2005-05-272006-11-30Prospex Medical Ii, Inc.Devices and methods for treating sleep disorders
US20060271137A1 (en)2005-05-252006-11-30The Cleveland Clinic FoundationApparatus and system to stimulate a nerve
US7149573B2 (en)2003-04-252006-12-12Medtronic, Inc.Method and apparatus for impedance signal localizations from implanted devices
US20060282127A1 (en)2005-03-242006-12-14Vanderbilt UniversityRespiratory triggered, bilateral laryngeal stimulator to restore normal ventilation in vocal fold paralysis
US7155278B2 (en)2003-04-212006-12-26Medtronic, Inc.Neurostimulation to treat effects of sleep apnea
US7152604B2 (en)2000-06-132006-12-26Scott Laboratories, Inc.Apparatus and method for mask free delivery of an inspired gas mixture and gas sampling
US20060293723A1 (en)2003-12-192006-12-28Whitehurst Todd KSkull-mounted electrical stimulation system and method for treating patients
US20060293720A1 (en)1998-08-052006-12-28Dilorenzo Daniel JClosed-loop feedback-driven neuromodulation
US7156098B2 (en)2004-03-192007-01-02Dolezal Creative Innovations, LlcBreathing air filtration system
US7160255B2 (en)2001-07-122007-01-09Vahid SaadatMethod and device for sensing and mapping temperature profile of a hollow body organ
US7160252B2 (en)2003-01-102007-01-09Medtronic, Inc.Method and apparatus for detecting respiratory disturbances
US20070021785A1 (en)2005-07-212007-01-25Cyberonics, Inc.Safe-mode implantable medical devices
JP2007021156A (en)2005-07-192007-02-01Isao MiyagawaTool for preventing invasion of pollen in nose
US20070027482A1 (en)2005-07-272007-02-01Cyberonics, Inc.Cranial nerve stimulation to treat a vocal cord disorder
US20070038265A1 (en)2002-02-052007-02-15Neuropace, Inc.Responsive electrical stimulation for movement disorders
US7178524B2 (en)1998-10-302007-02-20Linda NobleNasal gas delivery system and method for use thereof
US20070043411A1 (en)2005-08-172007-02-22Enteromedics Inc.Neural electrode
US7225034B2 (en)2003-06-192007-05-29Medtronic, Inc.Medical lead adaptor
US20070125379A1 (en)2005-12-022007-06-07Brian PierroNasal continuous positive airway pressure device and system
US20070150006A1 (en)*2005-12-282007-06-28Imad LibbusNeural stimulator to treat sleep disordered breathing
US7239920B1 (en)2002-02-122007-07-03Advanced Bionics CorporationNeural stimulation system providing auto adjustment of stimulus output as a function of sensed pressure changes
US20070175478A1 (en)2006-02-012007-08-02Brunst Robert FNasal air purifier
US20070227542A1 (en)2005-05-172007-10-04Boris KashmakovNose Filter
US20070239243A1 (en)2006-03-302007-10-11Advanced Bionics CorporationElectrode contact configurations for cuff leads
EP1854494A1 (en)2006-05-122007-11-14Intersurgical AGImprovements Relating to Respiratory Masks
WO2007134458A1 (en)2006-05-232007-11-29Jean-Pierre RobitailleValved nasal cannula
US20070277832A1 (en)2006-05-232007-12-06Ventus Medical, Inc.Nasal respiratory devices
US20070282410A1 (en)2006-04-282007-12-06Cross Thomas E JrImplantable medical lead assemblies with improved flexibility and extensibility and having a substantially two-dimensional nature
US20070283962A1 (en)2006-06-072007-12-13Ventus Medical, Inc.Layered nasal devices
US20070283692A1 (en)2006-06-092007-12-13Shimano Inc.Bicycle hydraulic brake accentuate device
US20070295338A1 (en)2004-12-082007-12-27Ventus Medical, Inc.Nasal respiratory devices for positive end-expiratory pressure
US20080027480A1 (en)2006-06-292008-01-31Aspire Medical, Inc.Methods and devices for rhinoplasty and treating internal valve stenosis
US20080023007A1 (en)2004-03-192008-01-31Dolezal David MBreathing air filtration devices
US20080027502A1 (en)2006-07-282008-01-31Ransom Scott ADynamic Sampling
WO2008046190A1 (en)2006-09-192008-04-24Victhom Human Bionics Inc.Method and system for the monitoring of respiratory activity and for the treatment of breathing disorders such as sleep apnea
US20080103407A1 (en)2006-10-132008-05-01Apnex Medical, Inc.Obstructive sleep apnea treatment devices, systems and methods
US20080099029A1 (en)2005-10-072008-05-01Lamberg Steven BIntraoral mandibular advancement device for treatment of sleep disorders
US20080147142A1 (en)*2006-12-152008-06-19Testerman Roy LMethod and apparatus for assisting deglutition
US20080163875A1 (en)2006-12-152008-07-105I Sciences, Inc.Device and method for opening an airway
US20080183254A1 (en)2007-01-302008-07-31Cardiac Pacemakers, Inc.Dual spiral lead configurations
US20090044814A1 (en)2007-06-182009-02-19Koninklijke Philips Electronics N.V.Implantable devices, systems, and methods for maintaining desired orientations in targeted tissue regions
US7515968B2 (en)2006-04-282009-04-07Medtronic, Inc.Assembly method for spinal cord stimulation lead
US7524292B2 (en)2003-04-212009-04-28Medtronic, Inc.Method and apparatus for detecting respiratory disturbances
US7591265B2 (en)2003-09-182009-09-22Cardiac Pacemakers, Inc.Coordinated use of respiratory and cardiac therapies for sleep disordered breathing
US7596413B2 (en)2004-06-082009-09-29Cardiac Pacemakers, Inc.Coordinated therapy for disordered breathing including baroreflex modulation
US7596414B2 (en)2005-12-052009-09-29Boston Scientific Neuromodulation CorporationCuff electrode arrangement for nerve stimulation and methods of treating disorders
US20090270707A1 (en)2008-04-232009-10-29Medtronic, Inc.Sensor Assemblies for Implantable Medical Electrical Leads
US20090276024A1 (en)2008-05-022009-11-05Bonde Eric HSelf expanding electrode cuff
US7627375B2 (en)2000-09-182009-12-01Cameron Health, Inc.Implantable cardiac stimulus methods
US7630771B2 (en)2007-06-252009-12-08Microtransponder, Inc.Grooved electrode and wireless microtransponder system
US7634315B2 (en)2007-05-312009-12-15Pacesetter, Inc.Techniques to monitor and trend nerve damage and recovery
US20090318986A1 (en)2008-06-202009-12-24Alo Kenneth MSystems, Methods and Apparatus for Treating Cardiac Dysfunction with Neurostimulation
US20090326408A1 (en)2008-06-302009-12-31Loell Boyce MoonProviding Impedance Plethysmography Electrodes
US7657311B2 (en)2000-09-182010-02-02Cameron Health, Inc.Subcutaneous only implantable cardioverter-defibrillator and optional pacer
US7660632B2 (en)2006-06-302010-02-09Ric Investments, LlcMethod and apparatus for hypoglossal nerve stimulation
US20100036285A1 (en)2008-08-062010-02-11Assaf GovariSingle-axis sensors on flexible backbone
US7662105B2 (en)2005-12-142010-02-16Cardiac Pacemakers, Inc.Systems and methods for determining respiration metrics
US20100047376A1 (en)2006-08-292010-02-25Marc-Olivier ImbeauNerve cuff injection mold and method of making a nerve cuff
US7684869B2 (en)2001-12-042010-03-23Boston Scientific Neuromodulation CorporationApparatus and method for determining the relative position and orientation of neurostimulation leads
US20100076536A1 (en)2006-09-222010-03-25Koninklijke Philips Electronics N.V.Implantable multi-electrode device
US7697968B2 (en)2006-03-282010-04-13Kent MooreSystem and method of predicting efficacy of tongue-base therapies
US7697990B2 (en)2004-02-202010-04-13Resmed LimitedMethod and apparatus for detection and treatment of respiratory disorder by implantable device
US20100094379A1 (en)2008-10-092010-04-15Imthera Medical, Inc.Method of Stimulating a Hypoglossal Nerve for Controlling the Position of a Patient's Tongue
US20100125310A1 (en)2008-11-182010-05-20Willard WilsonMethod and Device For the Detection, Identification and Treatment of Sleep Apnea/Hypopnea
US7725198B2 (en)2007-04-302010-05-25Medtronic, Inc.Implantable medical lead assemblies with delivery tether
US7725195B2 (en)2006-02-162010-05-25Imthera Medical, Inc.RFID-based apparatus, system, and method for therapeutic treatment of obstructive sleep apnea
US20100137949A1 (en)2008-05-272010-06-03The Cleveland Clinic FoundationBifurcated electrical lead and method of use
US20100137931A1 (en)2005-02-282010-06-03Hopper Donald LImplantable Cardiac Device With Dyspnea Measurement
US20100137956A1 (en)2001-10-222010-06-03Oscor Inc.Lead adaptor having low resistance conductors and/or encapsulated housing
US7734348B2 (en)2005-05-102010-06-08Cardiac Pacemakers, Inc.System with left/right pulmonary artery electrodes
US7747323B2 (en)2004-06-082010-06-29Cardiac Pacemakers, Inc.Adaptive baroreflex stimulation therapy for disordered breathing
US7751880B1 (en)2007-02-122010-07-06Pacesetter, Inc.Shielded electrode assembly for effective nerve sensing and stimulation
US7751885B2 (en)2000-09-182010-07-06Cameron Health, Inc.Bradycardia pacing in a subcutaneous device
US20100174341A1 (en)2008-12-312010-07-08Bolea Stephen LObstructive Sleep Apnea Treatment Devices, Systems and Methods
US7758384B2 (en)2007-02-262010-07-20Medtronic, Inc.Implantable bifurcated neurostimulator adapters
US7765000B2 (en)2005-05-102010-07-27Cardiac Pacemakers, Inc.Neural stimulation system with pulmonary artery lead
US7783353B2 (en)2003-12-242010-08-24Cardiac Pacemakers, Inc.Automatic neural stimulation modulation based on activity and circadian rhythm
US7787959B1 (en)2006-12-222010-08-31Pacesetter, Inc.Mechanism and method of attaching a stimulation and/or sensing electrode to a nerve
US7792590B1 (en)2000-12-292010-09-07Boston Scientific Neuromodulation CorporationImplantable lead systems for brain stimulation
US20100228133A1 (en)2005-09-162010-09-09Averina Viktoria ASystem and Method for Generating a Trend Parameter Based on Respiration Rate Distribution
US20100241207A1 (en)2006-08-142010-09-23Henry BlugerImplantable Medical Cuff with Electrode Array
US7813797B2 (en)2000-09-182010-10-12Cameron Health, Inc.Cardioverter-defibrillator having a focused shocking area and orientation thereof
US20100262209A1 (en)2002-02-122010-10-14Boston Scientific Neuromodulation CorporationNeural stimulation system providing auto adjustment of stimulus output as a function of sensed impedance
US7818063B2 (en)2003-12-222010-10-19Boston Scientific Scimed, Inc.Method of intravascularly delivering stimulation leads into brain to stimulate the SPG
US20110093032A1 (en)2009-08-052011-04-21Ndi Medical, LlcSystems and methods for maintaining airway patency
US20120022389A1 (en)2004-02-262012-01-26Linguaflex, Inc.Method and Device for the Treatment of Obstructive Sleep Apnea and Snoring
US20120192874A1 (en)2011-01-282012-08-02Apnex Medical, Inc.Obstructive sleep apnea treatment devices, systems and methods
US8249723B2 (en)2006-09-272012-08-21Huntington Medical Research InstitutesApparatus and method for treating obstructive sleep apnea
US20130085546A1 (en)2011-05-122013-04-04Stephen BoleaDevices and methods for sleep apnea treatment
US8855771B2 (en)2011-01-282014-10-07Cyberonics, Inc.Screening devices and methods for obstructive sleep apnea therapy
US9186511B2 (en)2006-10-132015-11-17Cyberonics, Inc.Obstructive sleep apnea treatment devices, systems and methods

Family Cites Families (13)

* Cited by examiner, † Cited by third party
Publication numberPriority datePublication dateAssigneeTitle
DE3278481D1 (en)*1982-03-191988-06-16Mettler Instrumente AgMeasuring instrument display, particularly for a balance
US5921942A (en)1995-11-011999-07-13University Technologies International, Inc.Adaptively controlled mandibular positioning device and method of using the device
US5927653A (en)1996-04-171999-07-27Kistler Aerospace CorporationTwo-stage reusable earth-to-orbit aerospace vehicle and transport system
US5988171A (en)*1997-06-261999-11-23Influence Medical Technologies, Ltd.Methods and devices for the treatment of airway obstruction, sleep apnea and snoring
US6269703B1 (en)1998-09-112001-08-07Femtometrics, Inc.Pulsed air sampler
US7203548B2 (en)2002-06-202007-04-10Advanced Bionics CorporationCavernous nerve stimulation via unidirectional propagation of action potentials
US7292890B2 (en)2002-06-202007-11-06Advanced Bionics CorporationVagus nerve stimulation via unidirectional propagation of action potentials
US7499755B2 (en)2002-10-232009-03-03Medtronic, Inc.Paddle-style medical lead and method
US20040215283A1 (en)2003-04-232004-10-28Antoine CampsElectrical stimulation of the colon to treat chronic constipation
JP4414800B2 (en)*2004-03-252010-02-10株式会社日立コミュニケーションテクノロジー Optical transmission apparatus and control method thereof
WO2006012050A2 (en)2004-06-302006-02-02Cvrx, Inc.Connection structures for extra-vascular electrode lead body
US7953498B1 (en)2006-03-152011-05-31Boston Scientific Neuromodulation CorporationResorbable anchor arrangements for implantable devices and methods of making and using
EP2310084B1 (en)*2008-05-022016-03-23Medtronic, Inc.Electrode lead system

Patent Citations (464)

* Cited by examiner, † Cited by third party
Publication numberPriority datePublication dateAssigneeTitle
US758030A (en)1903-06-301904-04-19Thomas CarenceNasal shield.
US1520930A (en)1923-09-011924-12-30Harry L CalhounFilter
US1701277A (en)1927-02-181929-02-05Willson Products IncValve device for respirators or the like
US1914418A (en)1930-02-151933-06-20Goyena Manuel GarciaNose protector
US2046664A (en)1935-11-071936-07-07Nasal Filter CoNasal filter
US2151227A (en)1937-02-121939-03-21Pawelek AnthonyNasal insert
US2243360A (en)1938-12-301941-05-27Slatis AbrahamFilter or medicament casing
US2237954A (en)1939-06-301941-04-08William R WilsonNasal filter and inhaler
US2274886A (en)1940-08-101942-03-03Harold D CarrollNasal respirator
US2526586A (en)1949-09-201950-10-17Leonard M ShuffNasal filter
US2693799A (en)1950-03-161954-11-09Jr Harry H HermanBreathing attachment for swimmers
US2777442A (en)1955-04-111957-01-15Zelano JosephNasal filter
US2928388A (en)1957-04-241960-03-15Alfred P JaroslawDisposable respirators
US3457917A (en)1966-02-171969-07-29John A MercurioNasal filtering device
US3513839A (en)1968-01-021970-05-26Matthew VacanteValved nose filter
US3680555A (en)1969-03-201972-08-01Draegerwerk AgProtective mask with annular flushing chamber
US3722509A (en)1971-01-051973-03-27J NebelNasal filters
US3774618A (en)1972-07-031973-11-27Avery Labor IncImplantable nerve stimulation electrode
US3893463A (en)1973-12-071975-07-08Medtronic IncDual channel stimulator
US3906936A (en)1974-02-151975-09-23Mutaz B HabalNasal air flow detection method for speech evaluation
US3865106A (en)1974-03-181975-02-11Bernard P PalushPositive pressure breathing circuit
US3884223A (en)1974-06-261975-05-20Lawrence Peska Ass IncNasal filter
US4178524A (en)1976-09-011979-12-11Ritter James CRadioisotope photoelectric generator
US4160255A (en)1976-10-041979-07-03Mitogiken, Ltd.Recording apparatus with intermittent power usage
US4160252A (en)1977-03-251979-07-03U.S. Philips CorporationMethod of determining the direction of a radio source and radio interferometer system
JPS53118893A (en)1977-03-281978-10-17Univ Case Western ReserveContinuous proper air path pressure feeder
US4242987A (en)1977-07-121981-01-06Hans ViessmannConnecting arrangement for a heating boiler
US4221217A (en)1978-05-011980-09-09Amezcua Saul ONasal device
US4225034A (en)1978-07-031980-09-30The Sardee CorporationContainer conveying and elevating apparatus
US4374527A (en)1978-07-191983-02-22Medtronic, Inc.Body stimulation lead
US4220150A (en)1978-09-131980-09-02King John RNasal dust filter
US4239918A (en)1978-12-061980-12-16General Electric CompanyMeta, para-substituted isopropylidene bisphenols and methods for making
US4200440A (en)1979-02-211980-04-29The Air Preheater Company, Inc.Filter construction
US4267831A (en)1979-09-241981-05-19Aguilar Rogelio MNasal air filter and medicament dispenser device
US4283867A (en)1979-12-051981-08-18Roscoe Brown CorporationBackfilling apparatus with adjustable filling augers
US4302951A (en)1979-12-261981-12-01Borg-Warner CorporationTorsional vibration damper
US4313442A (en)1980-07-211982-02-02Cardiac Pacemakers, Inc.Atrial rate sensitive cardiac pacer apparatus
US4346398A (en)1980-10-271982-08-24Zenith Radio CorporationAutomatic clock phase selector
US4612934A (en)1981-06-301986-09-23Borkan William NNon-invasive multiprogrammable tissue stimulator
US4414986A (en)1982-01-291983-11-15Medtronic, Inc.Biomedical stimulation lead
US4567892A (en)1982-03-161986-02-04Gianni PlicchiImplantable cardiac pacemaker
US4506666A (en)1982-12-031985-03-26Kircaldie, Randall And McnabMethod and apparatus for rectifying obstructive apnea
US4573481A (en)1984-06-251986-03-04Huntington Institute Of Applied ResearchImplantable electrode array
US4602624A (en)1984-10-111986-07-29Case Western Reserve UniversityImplantable cuff, method of manufacture, and method of installation
US5485836A (en)1987-03-201996-01-23Lincoln; Robert A.Nose worn air filter
US5036862A (en)1987-04-061991-08-06Cordis CorporationImplantable, self-retaining lead
US4830008A (en)1987-04-241989-05-16Meer Jeffrey AMethod and system for treatment of sleep apnea
US4777963A (en)1987-06-181988-10-18Mckenna KevinRespiration monitor
US5522382A (en)1987-06-261996-06-04Rescare LimitedDevice and method for treating obstructed breathing having a delay/ramp feature
US4919136A (en)1987-09-281990-04-24Eckhard AltVentilation controlled rate responsive cardiac pacemaker
US4934368A (en)1988-01-211990-06-19Myo/Kinetics Systems, Inc.Multi-electrode neurological stimulation apparatus
US4899750A (en)1988-04-191990-02-13Siemens-Pacesetter, Inc.Lead impedance scanning system for pacemakers
US4915105A (en)1988-10-281990-04-10Lee Tien ChuMiniature respiratory apparatus
US4960133A (en)1988-11-211990-10-02Brunswick Manufacturing Co., Inc.Esophageal electrode
US4940065A (en)1989-01-231990-07-10Regents Of The University Of CaliforniaSurgically implantable peripheral nerve electrode
US4996983A (en)1989-01-311991-03-05Amrhein Floyd EInhaler filtration device with housing supportable by spectacle temple
US5277193A (en)1989-06-201994-01-11Chest CorporationAPNEA preventive stimulating device
US5178156A (en)1989-06-201993-01-12Chest CorporationApnea preventive stimulating device
US5016808A (en)1989-09-141991-05-21Cardiac Pacemakers, Inc.Implantable tapered spiral endocardial lead for use in internal defibrillation
US4979511A (en)1989-11-031990-12-25Cyberonics, Inc.Strain relief tether for implantable electrode
US5095905A (en)1990-06-071992-03-17Medtronic, Inc.Implantable neural electrode
US5282468A (en)1990-06-071994-02-01Medtronic, Inc.Implantable neural electrode
US5121754A (en)1990-08-211992-06-16Medtronic, Inc.Lateral displacement percutaneously inserted epidural lead
US5105826A (en)1990-10-261992-04-21Medtronic, Inc.Implantable defibrillation electrode and method of manufacture
US5158080A (en)1990-11-081992-10-27Medtronic, Inc.Muscle tone
US5133354A (en)1990-11-081992-07-28Medtronic, Inc.Method and apparatus for improving muscle tone
US5281219A (en)1990-11-231994-01-25Medtronic, Inc.Multiple stimulation electrodes
US5211173A (en)1991-01-091993-05-18Medtronic, Inc.Servo muscle control
US5300094A (en)1991-01-091994-04-05Medtronic, Inc.Servo muscle control
US5190053A (en)1991-02-281993-03-02Jeffrey A. Meer, Revocable Living TrustMethod and apparatus for electrical sublingual stimulation
US5146918A (en)1991-03-191992-09-15Medtronic, Inc.Demand apnea control of central and obstructive sleep apnea
US5215082A (en)1991-04-021993-06-01Medtronic, Inc.Implantable apnea generator with ramp on generator
US5335657A (en)1991-05-031994-08-09Cyberonics, Inc.Therapeutic treatment of sleep disorder by nerve stimulation
US5174287A (en)1991-05-281992-12-29Medtronic, Inc.Airway feedback measurement system responsive to detected inspiration and obstructive apnea event
US5388578A (en)1992-01-141995-02-14Incontrol, Inc.Electrode system for use with an implantable cardiac patient monitor
US5511543A (en)1992-08-181996-04-30Shirley; Terry L.Disposable resuscitation device having unidirectional valve
US5324321A (en)1992-12-221994-06-28Medtronic, Inc.Medical electrical lead having sigmoidal conductors and non-circular lumens
US5630411A (en)1993-01-121997-05-20Nellcor Puritan Bennett IncorporatedValve for use with inhalation/exhalation respiratory phase detection circuit
US5344438A (en)1993-04-161994-09-06Medtronic, Inc.Cuff electrode
US5458629A (en)1994-02-181995-10-17Medtronic, Inc.Implantable lead ring electrode and method of making
US5392773A (en)1994-04-131995-02-28Bertrand; Archie A.Respiratory particulate filter
US5740798A (en)1994-04-221998-04-21Mckinney; Stella H.Disposable nasal band filter
US5417205A (en)1994-06-071995-05-23Wang; Jen-YiAir filter for the nose
US5787884A (en)1994-08-261998-08-04The University Of SydneyNasal and oral filters
US6109262A (en)1994-08-262000-08-29University Of SydneyNasal and oral filters
US5425359A (en)1994-08-291995-06-20Liou; Nan-TienNose plug structure with filter
US5919220A (en)1994-09-161999-07-06Fraunhofer Gesellschaft Zur Foerderung Der Angewandten Forschung E.V.Cuff electrode
US5531778A (en)1994-09-201996-07-02Cyberonics, Inc.Circumneural electrode assembly
US5485851A (en)1994-09-211996-01-23Medtronic, Inc.Method and apparatus for arousal detection
US5540732A (en)1994-09-211996-07-30Medtronic, Inc.Method and apparatus for impedance detecting and treating obstructive airway disorders
US5540733A (en)1994-09-211996-07-30Medtronic, Inc.Method and apparatus for detecting and treating obstructive sleep apnea
US5549655A (en)1994-09-211996-08-27Medtronic, Inc.Method and apparatus for synchronized treatment of obstructive sleep apnea
US5855552A (en)1994-09-211999-01-05Ep Technologies, Inc.Catheter having ring electrodes secured thereon
US5540731A (en)*1994-09-211996-07-30Medtronic, Inc.Method and apparatus for pressure detecting and treating obstructive airway disorders
US5522862A (en)1994-09-211996-06-04Medtronic, Inc.Method and apparatus for treating obstructive sleep apnea
US5483969A (en)1994-09-211996-01-16Medtronic, Inc.Method and apparatus for providing a respiratory effort waveform for the treatment of obstructive sleep apnea
US5540734A (en)1994-09-281996-07-30Zabara; JacobCranial nerve stimulation treatments using neurocybernetic prosthesis
US5487756A (en)1994-12-231996-01-30Simon Fraser UniversityImplantable cuff having improved closure
US5591216A (en)1995-05-191997-01-07Medtronic, Inc.Method for treatment of sleep apnea by electrical stimulation
US6041780A (en)1995-06-072000-03-28Richard; Ron F.Pressure control for constant minute volume
US5568808A (en)1995-08-081996-10-29Amtec Products, IncorporatedNose filters
US5546938A (en)1995-08-241996-08-20Mckenzie; Shirley T.ICU patients ventilator tube holding device
US6205360B1 (en)1995-09-072001-03-20Cochlear LimitedApparatus and method for automatically determining stimulation parameters
US20020010495A1 (en)1995-10-272002-01-24Freed Marcy L.Method and apparatus for treating oropharyngeal, respiratory and oral motor neuromuscular disorders with electrical stimulation
US20030093128A1 (en)1995-10-272003-05-15Freed Marcy L.Method and apparatus for treating oropharyngeal, respiratory and oral motor neuromuscular disorders with electrical stimulation
US6198970B1 (en)1995-10-272001-03-06Esd Limited Liability CompanyMethod and apparatus for treating oropharyngeal respiratory and oral motor neuromuscular disorders with electrical stimulation
US6015389A (en)1995-12-062000-01-18Btg International LimitedImpedance pneumography
US6010459A (en)1996-04-092000-01-04Silkoff; Philip E.Method and apparatus for the measurement of components of exhaled breath in humans
EP0892926B1 (en)1996-04-092002-06-26Sievers Instruments, Inc.Method and apparatus for the measurement of components of exhaled breath in humans
JP2000506601A (en)1996-04-092000-05-30シーヴァース インストルメンツ,インコーポレーテッド Method and apparatus for measurement of human breath constituents
JP3688301B2 (en)1996-04-122005-08-24アルバート アインスタイン ヘルスケア ネットワーク Inhalation and monitoring device
US5697363A (en)1996-04-121997-12-16Albert Einstein Healthcare NetworkInhalation and monitoring mask with headset
JP2000508562A (en)1996-04-122000-07-11アルバート アインスタイン ヘルスケア ネットワーク Inhalation and monitoring device
EP0900102B1 (en)1996-04-122004-07-07Albert Einstein Healthcare NetworkInhalation and monitoring device
US20050251216A1 (en)1996-04-302005-11-10Medtronic, Inc.Method and device for electronically controlling the beating of a heart
US7697984B2 (en)1996-04-302010-04-13Medtronic, Inc.Method and device for electronically controlling the beating of a heart
USRE38705E1 (en)1996-04-302005-02-22Medtronic, Inc.Method and device for electronically controlling the beating of a heart using venous electrical stimulation of nerve fibers
JPH09294819A (en)1996-05-021997-11-18孝明 ▲崎▼Nose mask
US6609031B1 (en)1996-06-072003-08-19Advanced Neuromodulation Systems, Inc.Multiprogrammable tissue stimulator and method
US6021352A (en)1996-06-262000-02-01Medtronic, Inc,Diagnostic testing methods and apparatus for implantable therapy devices
US5944680A (en)1996-06-261999-08-31Medtronic, Inc.Respiratory effort detection method and apparatus
US5895360A (en)1996-06-261999-04-20Medtronic, Inc.Gain control for a periodic signal and method regarding same
US6132384A (en)1996-06-262000-10-17Medtronic, Inc.Sensor, method of sensor implant and system for treatment of respiratory disorders
US5697105A (en)1996-09-041997-12-16White; MarkHunting mask
US5682881A (en)1996-10-211997-11-04Winthrop; NeilNasal CPAP/Cannula and securement apparatus
WO1998020938A1 (en)1996-11-121998-05-22Cprx, Inc.Heart failure treatment method requiring set negative intrathoracic pressure
US5730122A (en)1996-11-121998-03-24Cprx, Inc.Heart failure mask and methods for increasing negative intrathoracic pressures
US6029667A (en)1996-11-122000-02-29Cprx LlcHeart failure mask and methods for increasing negative intrathoracic pressures
US5752511A (en)1996-11-221998-05-19Simmons; Carl J.Universal medical tube retainer and nasal wall tissue dilator
US6098624A (en)1996-12-162000-08-08Utamaru; MasanobuSimple mask for protection of respiratory system
US6366815B1 (en)1997-01-132002-04-02Neurodan A /SImplantable nerve stimulator electrode
US5938596A (en)1997-03-171999-08-17Medtronic, Inc.Medical electrical lead
US5922014A (en)1997-09-021999-07-13Medtronic, Inc.Single pass lead and method of use
US6021354A (en)1997-09-022000-02-01Medtronic, Inc.Single pass lead and method of use
US6201994B1 (en)1997-09-022001-03-13Medtronic, Inc.Single pass lead and method of use
US5890491A (en)1997-09-031999-04-06Amtec Products, Inc.Nose filter
US20030083696A1 (en)1997-09-032003-05-01Hadasit Medical Research Service & Development CompanyPacifier
US5848589A (en)1997-09-181998-12-15Welnetz; Robert J.Altitude mask simulator
US5871531A (en)1997-09-251999-02-16Medtronic, Inc.Medical electrical lead having tapered spiral fixation
US5947119A (en)1997-10-311999-09-07Reznick; Jerald M.Therapeutic process and apparatus for nasal passages
US7027869B2 (en)1998-01-072006-04-11Asthmatx, Inc.Method for treating an asthma attack
US6511458B2 (en)1998-01-132003-01-28Lumend, Inc.Vascular re-entry catheter
US6231546B1 (en)1998-01-132001-05-15Lumend, Inc.Methods and apparatus for crossing total occlusions in blood vessels
US6221049B1 (en)1998-01-132001-04-24Lumend, Inc.Methods and apparatus for crossing vascular occlusions
US6514217B1 (en)1998-01-132003-02-04Lumend, Inc.Methods and apparatus for treating vascular occlusions
US6719725B2 (en)1998-01-132004-04-13Lumend, Inc.Re-entry catheter
US20060129189A1 (en)1998-01-152006-06-15Regenesis Biomedical, Inc.Pulsed electromagnetic energy treatment apparatus and method
US6126611A (en)1998-02-042000-10-03Medtronic, Inc.Apparatus for management of sleep apnea
US6647289B2 (en)1998-02-062003-11-11Intermedics Inc.Non-invasive cardiorespiratory monitor with synchronized bioimpedance sensing
US6251126B1 (en)1998-04-232001-06-26Medtronic IncMethod and apparatus for synchronized treatment of obstructive sleep apnea
US6269269B1 (en)1998-04-232001-07-31Medtronic Inc.Method and apparatus for synchronized treatment of obstructive sleep apnea
US6066165A (en)1998-04-302000-05-23Racz; Gabor BMedical lead with sigma feature
US6651652B1 (en)1998-06-302003-11-25Siemens-Elema AbMethod for identifying respiration attempts by analyzing neuroelectrical signals, and respiration detector and respiratory aid system operating according to the method
US6587725B1 (en)1998-07-272003-07-01Dominique DurandMethod and apparatus for closed-loop stimulation of the hypoglossal nerve in human patients to treat obstructive sleep apnea
US20060293720A1 (en)1998-08-052006-12-28Dilorenzo Daniel JClosed-loop feedback-driven neuromodulation
US6240316B1 (en)1998-08-142001-05-29Advanced Bionics CorporationImplantable microstimulation system for treatment of sleep apnea
US20010010010A1 (en)1998-08-142001-07-26Richmond Francis J.R.Method of treating obstructive sleep apnea using implantable electrodes
US6345202B2 (en)1998-08-142002-02-05Advanced Bionics CorporationMethod of treating obstructive sleep apnea using implantable electrodes
US6217527B1 (en)1998-09-302001-04-17Lumend, Inc.Methods and apparatus for crossing vascular occlusions
US6292703B1 (en)1998-10-082001-09-18Biotronik Mess-Und Therapiegerate Gmbh & Co.Neural electrode arrangement
US7178524B2 (en)1998-10-302007-02-20Linda NobleNasal gas delivery system and method for use thereof
US6119690A (en)1998-12-042000-09-19Pantaleo; Joseph M.Nostril filter system
US6997177B2 (en)1999-03-132006-02-14Inno Med Technologies, Inc.Ventilation interface for sleep apnea therapy
US20050039757A1 (en)1999-03-132005-02-24Wood Thomas J.Ventilation interface for sleep apnea therapy
US20030114895A1 (en)1999-04-142003-06-19Transneuronix, Inc.Gastric stimulator apparatus and method for installing
US6542776B1 (en)1999-04-142003-04-01Transneuronix Inc.Gastric stimulator apparatus and method for installing
US7094206B2 (en)1999-04-232006-08-22The Trustees Of Tufts CollegeSystem for measuring respiratory function
US6244267B1 (en)1999-07-082001-06-12DRäGER MEDIZINTECHNICK GMBHRespirator with a pressure relief valve
US6636767B1 (en)1999-09-292003-10-21Restore Medical, Inc.Implanatable stimulation device for snoring treatment
US20040073272A1 (en)1999-09-292004-04-15Restore Medical, Inc.Implantable stimulation device for snoring treatment
US20050267547A1 (en)1999-09-292005-12-01Restore Medical, Inc.Microstimulator treatment for sleep apnea or snoring
US20030114905A1 (en)1999-10-012003-06-19Kuzma Janusz A.Implantable microdevice with extended lead and remote electrode
US20030106556A1 (en)1999-12-102003-06-12Vladimir AlperovichRespiratory nasal filter
US20010031929A1 (en)1999-12-282001-10-18O'toole JamesEnd tidal carbon dioxide sampling device
US20030106555A1 (en)2000-02-242003-06-12Euan ToveyNasal filter and sampler
US20020092527A1 (en)2000-03-132002-07-18Wood Thomas J.Ventilation interface for sleep apnea therapy
US6776162B2 (en)2000-03-132004-08-17Innomed Technologies, Inc.Ventilation interface for sleep apnea therapy
US20030034031A1 (en)2000-05-222003-02-20Sleep Up Ltd.Pacifier and method of use thereof
US20070095347A1 (en)2000-06-132007-05-03Scott Laboratories, Inc.Apparatus and method for mask free delivery of an inspired gas mixture and gas sampling
US7152604B2 (en)2000-06-132006-12-26Scott Laboratories, Inc.Apparatus and method for mask free delivery of an inspired gas mixture and gas sampling
US20060032497A1 (en)2000-06-162006-02-16Rajiv DoshiMethods and devices for improving breathing in patients with pulmonary disease
US6561188B1 (en)2000-08-212003-05-13Ellis Alan DNasal breathing apparatus and methods
US7627375B2 (en)2000-09-182009-12-01Cameron Health, Inc.Implantable cardiac stimulus methods
US7657311B2 (en)2000-09-182010-02-02Cameron Health, Inc.Subcutaneous only implantable cardioverter-defibrillator and optional pacer
US7065410B2 (en)2000-09-182006-06-20Cameron Health, Inc.Subcutaneous electrode with improved contact shape for transthorasic conduction
US7813797B2 (en)2000-09-182010-10-12Cameron Health, Inc.Cardioverter-defibrillator having a focused shocking area and orientation thereof
US7720534B2 (en)2000-09-182010-05-18Cameron Health, Inc.Transthoracic impedance measurement in a subcutaneous device
US7751885B2 (en)2000-09-182010-07-06Cameron Health, Inc.Bradycardia pacing in a subcutaneous device
WO2002024279A1 (en)2000-09-212002-03-283M Innovative Properties CompanyRespirator that includes an integral filter element, an exhalation valve, and impactor element
JP2004508908A (en)2000-09-212004-03-25スリーエム イノベイティブ プロパティズ カンパニー Ventilator with integrated filter element, exhalation valve and impactor element
US6460539B1 (en)2000-09-212002-10-083M Innovative Properties CompanyRespirator that includes an integral filter element, an exhalation valve, and impactor element
EP1322384B1 (en)2000-09-212007-12-193M Innovative Properties CompanyRespirator that includes an integral filter element, an exhalation valve, and impactor element
US6626179B1 (en)2000-09-292003-09-30Philip PedleyBreathing valve for improving oxygen absorption
US20020049479A1 (en)2000-10-202002-04-25Pitts Walter C.Method and apparatus for creating afferents to prevent obstructive sleep apnea
US6772015B2 (en)2000-12-292004-08-03Medtronic, IncBifurcated lead system for a cardiac vein
US7792590B1 (en)2000-12-292010-09-07Boston Scientific Neuromodulation CorporationImplantable lead systems for brain stimulation
US20020165462A1 (en)2000-12-292002-11-07Westbrook Philip R.Sleep apnea risk evaluation
US20040230278A1 (en)2000-12-292004-11-18Medtronic, Inc.Bifurcated lead system for a cardiac vein
US6876885B2 (en)2001-01-312005-04-05Medtronic, Inc.Implantable bifurcated gastrointestinal lead with active fixation
US6819958B2 (en)2001-02-202004-11-16Biophan Technologies, Inc.Electromagnetic interference immune tissue invasive system
US20020128700A1 (en)2001-03-082002-09-12Cross Thomas E.Lead with adjustable angular and spatial relationships between electrodes
US20020156507A1 (en)*2001-04-052002-10-24Werner LindenthalerPacemaker for bilateral vocal cord autoparalysis
US6799575B1 (en)2001-04-212004-10-05Aaron CarterCannula for the separation of inhaled and exhaled gases
US6641542B2 (en)2001-04-302003-11-04Medtronic, Inc.Method and apparatus to detect and treat sleep respiratory events
US6718982B2 (en)2001-05-072004-04-13Mark A. SmithFace mask incorporating respiratory flow sensor
US20020166556A1 (en)2001-05-092002-11-14Joseph JacobNose airflow enhancer and filter for airborne solids and pathogens
US20040215290A1 (en)*2001-06-212004-10-28Zealear David LMethod for promoting reinnervation of denervated tissue
US7054692B1 (en)2001-06-222006-05-30Advanced Bionics CorporationFixation device for implantable microdevices
US6484725B1 (en)2001-06-252002-11-26Min Hung ChiNose plug device having air breathing structure
US7302951B2 (en)2001-06-252007-12-043M Innovative Properties CompanyUnidirectional respirator valve
US20020195109A1 (en)2001-06-252002-12-263M Innovative Properties CompanyRespirator valve
WO2003000347A1 (en)2001-06-252003-01-033M Innovative Properties CompanyRespirator valve
US20020195108A1 (en)2001-06-252002-12-263M Innovative Properties CompanyRespirator valve
JP2004532707A (en)2001-06-252004-10-28スリーエム イノベイティブ プロパティズ カンパニー Breathing device valve
US6883518B2 (en)2001-06-252005-04-263M Innovative Properties CompanyUnidirectional respirator valve
US20050139216A1 (en)2001-06-252005-06-303M Innovative Properties CompanyUnidirectional respirator valve
US20040233058A1 (en)2001-06-262004-11-25Dennis DoddsRespiration monitoring equipment
US7089932B2 (en)2001-06-262006-08-15Dennis DoddsRespiration monitoring equipment
WO2003000133A1 (en)2001-06-262003-01-03C-Lect Medical LtdRespiration monitoring equipment
EP1404221A1 (en)2001-06-262004-04-07C-Lect Medical Ltd.Respiration monitoring equipment
US6606521B2 (en)2001-07-092003-08-12Neuropace, Inc.Implantable medical lead
US20050098176A1 (en)2001-07-122005-05-12Helmut HoffrichterRespiratory therapy device for keeping free the natural respiratory tract of a human body and the use thereof in order to prevent the sound of snoring
US7160255B2 (en)2001-07-122007-01-09Vahid SaadatMethod and device for sensing and mapping temperature profile of a hollow body organ
US6600956B2 (en)2001-08-212003-07-29Cyberonics, Inc.Circumneural electrode assembly
US20030040785A1 (en)2001-08-212003-02-27Maschino Steve E.Circumneural electrode assembly
US7346398B2 (en)2001-08-312008-03-18Bio Control Medical (B.C.M.) Ltd.Electrode assembly for nerve control
US20050038490A1 (en)2001-08-312005-02-17Biocontrol Medical Ltd.Electrode assembly for nerve control
US6907295B2 (en)2001-08-312005-06-14Biocontrol Medical Ltd.Electrode assembly for nerve control
US20040116819A1 (en)2001-10-012004-06-17Eckhard AltCongestive heart failure monitor and ventilation measuring implant
US6829503B2 (en)2001-10-012004-12-07Scicotec GmbhCongestive heart failure monitor
US20030078643A1 (en)2001-10-192003-04-24Schulman Joseph H.Electrically sensing and stimulating system for placement of a nerve stimulator or sensor
US6829508B2 (en)2001-10-192004-12-07Alfred E. Mann Foundation For Scientific ResearchElectrically sensing and stimulating system for placement of a nerve stimulator or sensor
US20100137956A1 (en)2001-10-222010-06-03Oscor Inc.Lead adaptor having low resistance conductors and/or encapsulated housing
US7684869B2 (en)2001-12-042010-03-23Boston Scientific Neuromodulation CorporationApparatus and method for determining the relative position and orientation of neurostimulation leads
US6890306B2 (en)2001-12-142005-05-10Ela Medical S.A.Active medical device for the diagnosis of the sleep apnea syndrome
US6721603B2 (en)2002-01-252004-04-13Cyberonics, Inc.Nerve stimulation as a treatment for pain
US7813802B2 (en)2002-02-052010-10-12Neuropace, Inc.Responsive electrical stimulation for movement disorders
US20070038265A1 (en)2002-02-052007-02-15Neuropace, Inc.Responsive electrical stimulation for movement disorders
US20100262209A1 (en)2002-02-122010-10-14Boston Scientific Neuromodulation CorporationNeural stimulation system providing auto adjustment of stimulus output as a function of sensed impedance
US7239920B1 (en)2002-02-122007-07-03Advanced Bionics CorporationNeural stimulation system providing auto adjustment of stimulus output as a function of sensed pressure changes
US6904320B2 (en)2002-02-142005-06-07Pacesetter, Inc.Sleep apnea therapy device using dynamic overdrive pacing
US20030209145A1 (en)2002-02-142003-11-13Soper Adrian JohnFiltration device
US20030153953A1 (en)*2002-02-142003-08-14Euljoon ParkStimulation device for sleep apnea prevention, detection and treatment
US6928324B2 (en)2002-02-142005-08-09Pacesetter, Inc.Stimulation device for sleep apnea prevention, detection and treatment
US20030167018A1 (en)2002-03-042003-09-04Robert WyckoffSleep apnea device and method thereof
US6978171B2 (en)2002-03-152005-12-20Medtronic, Inc.Automated impedance measurement of an implantable medical device
US20050235992A1 (en)2002-03-282005-10-27Djupesland Per GNasal devices
WO2003082393A1 (en)2002-03-282003-10-09Optinose AsNasal devices
JP2005521485A (en)2002-03-282005-07-21オプティノーズ アズ Nasal device
US20050234523A1 (en)2002-04-082005-10-20Levin Howard RRenal nerve stimulation method and apparatus for treatment of patients
US20030195571A1 (en)2002-04-122003-10-16Burnes John E.Method and apparatus for the treatment of central sleep apnea using biventricular pacing
JP2003305135A (en)2002-04-172003-10-28Takao AkeuraBandage type nose mask
US20060079802A1 (en)2002-04-302006-04-13Medtronic, Inc.Method and apparatus to detect and monitor the frequency of obstructive sleep apnea
US20030216789A1 (en)2002-05-142003-11-20The Foundry, Inc.Method and system for treating sleep apnea
US20060195170A1 (en)2002-05-232006-08-31Ehud CohenElectrode assembly for nerve control
US20060116739A1 (en)2002-05-232006-06-01Nir BetserElectrode assembly for nerve control
US20060211951A1 (en)2002-05-292006-09-21Zoran MilijasevicImplantable bladder sensor
US6881192B1 (en)2002-06-122005-04-19Pacesetter, Inc.Measurement of sleep apnea duration and evaluation of response therapies using duration metrics
US7860570B2 (en)2002-06-202010-12-28Boston Scientific Neuromodulation CorporationImplantable microstimulators and methods for unidirectional propagation of action potentials
US20040015204A1 (en)2002-06-202004-01-22Whitehurst Todd K.Implantable microstimulators and methods for unidirectional propagation of action potentials
US7117036B2 (en)2002-06-272006-10-03Pacesetter, Inc.Using activity-based rest disturbance as a metric of sleep apnea
US20060064029A1 (en)2002-07-032006-03-23Tel-Aviv University Future Technology Development L.P.Bio-impedance apparatus and method
US20040020489A1 (en)2002-07-252004-02-05Gail AlstonNasal mask with replaceable filter
US20040049241A1 (en)2002-09-102004-03-11Therapeutic Innovations, Inc.Distributed muscle stimulator
US20040055603A1 (en)2002-09-232004-03-25Bruce Carol Jean EmeryIntra-nasal filter device
US20040162499A1 (en)2002-10-042004-08-19Fumiya NagaiAbnormal respiration detecting system and method for detecting the same
US20040138581A1 (en)2002-10-152004-07-15Medtronic, Inc.Signal quality monitoring and control for a medical device system
US7797057B2 (en)2002-10-232010-09-14Medtronic, Inc.Medical paddle lead and method for spinal cord stimulation
US20040260310A1 (en)2002-10-232004-12-23Medtronic, Inc.Medical lead and method
US20040089303A1 (en)2002-11-112004-05-13Dennis ChienNose filter device
US20040116978A1 (en)2002-12-062004-06-17Kerry BradleyMethod for determining stimulation parameters
US20040111139A1 (en)2002-12-102004-06-10Mccreery Douglas B.Apparatus and methods for differential stimulation of nerve fibers
US20040122497A1 (en)2002-12-192004-06-24Yongxing ZhangImplantable lead for septal placement of electrode with fixation mechanism in the pulmonary artery
US7438686B2 (en)2003-01-102008-10-21Medtronic, Inc.Apparatus and method for monitoring for disordered breathing
US20050119711A1 (en)2003-01-102005-06-02Cho Yong K.Apparatus and method for monitoring for disordered breathing
US7160252B2 (en)2003-01-102007-01-09Medtronic, Inc.Method and apparatus for detecting respiratory disturbances
US7277749B2 (en)2003-01-152007-10-02Alfred E. Mann Institute For Biomedical Engineering At The University Of Southern CaliforniaTreatments for snoring using injectable neuromuscular stimulators
US20040153127A1 (en)2003-01-152004-08-05Alfred E. Mann Institute For Biomedical Engineering At The University Of Southern CalifornTreatments for snoring using injectable neuromuscular stimulators
US20040194784A1 (en)2003-04-012004-10-07Archie BertrandRespiratory particulate filter
US7636602B2 (en)2003-04-022009-12-22Neurostream Technologies General PartnershipFully implantable nerve signal sensing and stimulation device and method for treating foot drop and other neurological disorders
US20050010265A1 (en)2003-04-022005-01-13Neurostream Technologies Inc.Fully implantable nerve signal sensing and stimulation device and method for treating foot drop and other neurological disorders
US7524292B2 (en)2003-04-212009-04-28Medtronic, Inc.Method and apparatus for detecting respiratory disturbances
US7155278B2 (en)2003-04-212006-12-26Medtronic, Inc.Neurostimulation to treat effects of sleep apnea
US7463928B2 (en)2003-04-252008-12-09Medtronic, Inc.Identifying combinations of electrodes for neurostimulation therapy
US20040215288A1 (en)2003-04-252004-10-28Lee Michael T.Identifying combinations of electrodes for neurostimulation therapy
US7149573B2 (en)2003-04-252006-12-12Medtronic, Inc.Method and apparatus for impedance signal localizations from implanted devices
US20050261747A1 (en)2003-05-162005-11-24Schuler Eleanor LMethod and system to control respiration by means of neuro-electrical coded signals
US20060111755A1 (en)2003-05-162006-05-25Stone Robert TMethod and system to control respiration by means of neuro-electrical coded signals
US20060224209A1 (en)2003-05-162006-10-05Dennis MeyerMethod and system to control respiration by means of simulated neuro-electrical coded signals
US20050240241A1 (en)2003-06-092005-10-27Yun Anthony JTreatment of conditions through modulation of the autonomic nervous system
US7738952B2 (en)2003-06-092010-06-15Palo Alto InvestorsTreatment of conditions through modulation of the autonomic nervous system
US7242987B2 (en)2003-06-192007-07-10Medtronic, Inc.Medical lead adaptor
US7225034B2 (en)2003-06-192007-05-29Medtronic, Inc.Medical lead adaptor
US20040261791A1 (en)2003-06-242004-12-30Horian Richard C.Nasal dilator and method of nasal dilation
US7263996B2 (en)2003-07-022007-09-04Kim Yung HoAnion emission and anti-dust nose mask
US20060150980A1 (en)2003-07-022006-07-13Yung Ho KimAnion emission and anti-dust nose mask
US7200440B2 (en)2003-07-022007-04-03Cardiac Pacemakers, Inc.Cardiac cycle synchronized sampling of impedance signal
US20050004610A1 (en)2003-07-022005-01-06Jaeho KimCardiac cycle synchronized sampling of impedance signal
WO2005004993A1 (en)2003-07-122005-01-20Lixin ZhouA nasal filter
US20050043644A1 (en)2003-08-182005-02-24Stahmann Jeffrey E.Prediction of disordered breathing
US20050043772A1 (en)2003-08-182005-02-24Stahmann Jeffrey E.Therapy triggered by prediction of disordered breathing
US7680537B2 (en)2003-08-182010-03-16Cardiac Pacemakers, Inc.Therapy triggered by prediction of disordered breathing
US7396333B2 (en)2003-08-182008-07-08Cardiac Pacemakers, Inc.Prediction of disordered breathing
US7473227B2 (en)2003-09-022009-01-06Biotronik Gmbh & Co.KgApparatus for the treatment of sleep apnea
US20050101833A1 (en)2003-09-022005-05-12Biotronik Gmbh & Co. KgApparatus for the treatment of sleep apnea
US20060149345A1 (en)2003-09-122006-07-06Ndi Medical, LlcNeuromodulation stimulation for the restoration of sexual function
US7591265B2 (en)2003-09-182009-09-22Cardiac Pacemakers, Inc.Coordinated use of respiratory and cardiac therapies for sleep disordered breathing
US20090308395A1 (en)2003-09-182009-12-17Kent LeeCoordinated Use of Respiratory and Cardiac Therapies for Sleep Disordered Breathing
US20050076908A1 (en)2003-09-182005-04-14Kent LeeAutonomic arousal detection system and method
US20050085866A1 (en)2003-10-152005-04-21Tehrani Amir J.Breathing disorder and precursor predictor and therapy delivery device and method
US20050085865A1 (en)2003-10-152005-04-21Tehrani Amir J.Breathing disorder detection and therapy delivery device and method
US7979128B2 (en)2003-10-152011-07-12Rmx, LlcDevice and method for gradually controlling breathing
US20050085868A1 (en)2003-10-152005-04-21Tehrani Amir J.Breathing therapy device and method
US20050085869A1 (en)2003-10-152005-04-21Tehrani Amir J.System and method for mapping diaphragm electrode sites
US8255056B2 (en)2003-10-152012-08-28Rmx, LlcBreathing disorder and precursor predictor and therapy delivery device and method
US20060149334A1 (en)*2003-10-152006-07-06Tehrani Amir JDevice and method for controlling breathing
US20060142815A1 (en)2003-10-152006-06-29Tehrani Amir JDevice and method for treating obstructive sleep apnea
US20060247729A1 (en)2003-10-152006-11-02Tehrani Amir JMultimode device and method for controlling breathing
US20060155341A1 (en)2003-10-152006-07-13Tehrani Amir JDevice and method for biasing lung volume
US20050085874A1 (en)2003-10-172005-04-21Ross DavisMethod and system for treating sleep apnea
US7142919B2 (en)2003-10-242006-11-28Medtronic, Inc.Reconfigurable, fault tolerant multiple-electrode cardiac lead systems
US20060293723A1 (en)2003-12-192006-12-28Whitehurst Todd KSkull-mounted electrical stimulation system and method for treating patients
US7769461B2 (en)2003-12-192010-08-03Boston Scientific Neuromodulation CorporationSkull-mounted electrical stimulation system and method for treating patients
US7818063B2 (en)2003-12-222010-10-19Boston Scientific Scimed, Inc.Method of intravascularly delivering stimulation leads into brain to stimulate the SPG
US7783353B2 (en)2003-12-242010-08-24Cardiac Pacemakers, Inc.Automatic neural stimulation modulation based on activity and circadian rhythm
US20050165457A1 (en)2004-01-262005-07-28Michael BenserTiered therapy for respiratory oscillations characteristic of Cheyne-Stokes respiration
US20060004429A1 (en)2004-02-122006-01-05Ndi Medical, Inc.Lead and electrode structures sized and configured for implantation in adipose tissue and associated methods of implantation
US7343202B2 (en)2004-02-122008-03-11Ndi Medical, Llc.Method for affecting urinary function with electrode implantation in adipose tissue
US20100152553A1 (en)2004-02-202010-06-17Anthony John UjhazyMethod and apparatus for detection and treatment of respiratory disorder by implantable device
US7697990B2 (en)2004-02-202010-04-13Resmed LimitedMethod and apparatus for detection and treatment of respiratory disorder by implantable device
US20120017920A1 (en)2004-02-262012-01-26Linguaflex, Inc.Method and Device for the Treatment of Obstructive Sleep Apnea and Snoring
US20120022389A1 (en)2004-02-262012-01-26Linguaflex, Inc.Method and Device for the Treatment of Obstructive Sleep Apnea and Snoring
US20050209643A1 (en)2004-03-162005-09-22Heruth Kenneth TControlling therapy based on sleep quality
US7366572B2 (en)2004-03-162008-04-29Medtronic, Inc.Controlling therapy based on sleep quality
US7717848B2 (en)2004-03-162010-05-18Medtronic, Inc.Collecting sleep quality information via a medical device
US20050209513A1 (en)2004-03-162005-09-22Heruth Kenneth TCollecting sleep quality information via a medical device
US7156098B2 (en)2004-03-192007-01-02Dolezal Creative Innovations, LlcBreathing air filtration system
US20080023007A1 (en)2004-03-192008-01-31Dolezal David MBreathing air filtration devices
US20050267380A1 (en)2004-04-042005-12-01Ela Medical S.A.Active implantable medical device equipped with means for the diagnosis of respiratory disorders, with sophisticated detection of respiratory cycles with artifacts
US7082331B1 (en)2004-04-212006-07-25Pacesetter, Inc.System and method for applying therapy during hyperpnea phase of periodic breathing using an implantable medical device
US20060064138A1 (en)2004-04-302006-03-23Francisco VelascoMethod of treating mood disorders and/or anxiety disorders by brain stimulation
US7313442B2 (en)2004-04-302007-12-25Advanced Neuromodulation Systems, Inc.Method of treating mood disorders and/or anxiety disorders by brain stimulation
US7087053B2 (en)2004-05-272006-08-08St. Jude Medical, Atrial Fibrillation Division, Inc.Catheter with bifurcated, collapsible tip for sensing and ablating
US20100228317A1 (en)2004-06-082010-09-09Imad LibbusAdaptive baroreflex stimulation therapy for disordered breathing
US7596413B2 (en)2004-06-082009-09-29Cardiac Pacemakers, Inc.Coordinated therapy for disordered breathing including baroreflex modulation
US7747323B2 (en)2004-06-082010-06-29Cardiac Pacemakers, Inc.Adaptive baroreflex stimulation therapy for disordered breathing
US7283867B2 (en)2004-06-102007-10-16Ndi Medical, LlcImplantable system and methods for acquisition and processing of electrical signals from muscles and/or nerves and/or central nervous system tissue
US7813809B2 (en)2004-06-102010-10-12Medtronic, Inc.Implantable pulse generator for providing functional and/or therapeutic stimulation of muscles and/or nerves and/or central nervous system tissue
US7239918B2 (en)2004-06-102007-07-03Ndi Medical Inc.Implantable pulse generator for providing functional and/or therapeutic stimulation of muscles and/or nerves and/or central nervous system tissue
US20050278000A1 (en)2004-06-102005-12-15Strother Robert BImplantable pulse generator for providing functional and/or therapeutic stimulation of muscles and/or nerves and/or central nervous system tissue
US20050277844A1 (en)2004-06-102005-12-15Ndi Medical, Inc.Implantable system and methods for acquisition and processing of electrical signals from muscles and/or nerves and/or central nervous system tissue
US20050277999A1 (en)2004-06-102005-12-15Ndi Medical, LlcImplantable pulse generator for providing functional and/or therapeutic stimulation of muscles and /or nerves and/or central nervous system tissue
US20060005842A1 (en)2004-07-092006-01-12Rashad M ANasal pressure sensor oxygen therapy device
US20060025828A1 (en)2004-07-282006-02-02Armstrong Randolph KImpedance measurement for an implantable device
US20060030919A1 (en)2004-08-042006-02-09Ndi Medical, LlcDevices, systems, and methods employing a molded nerve cuff electrode
US7797058B2 (en)2004-08-042010-09-14Ndi Medical, LlcDevices, systems, and methods employing a molded nerve cuff electrode
US20060041295A1 (en)2004-08-172006-02-23Osypka Thomas PPositive fixation percutaneous epidural neurostimulation lead
US20060058588A1 (en)2004-09-022006-03-16Proteus Biomedical, Inc.Methods and apparatus for tissue activation and monitoring
US20060052836A1 (en)2004-09-082006-03-09Kim Daniel HNeurostimulation system
US7672729B2 (en)2004-09-102010-03-02Pacesetter, Inc.Multi-variable feedback control of stimulation for inspiratory facilitation
US20060058852A1 (en)2004-09-102006-03-16Steve KohMulti-variable feedback control of stimulation for inspiratory facilitation
US20060095088A1 (en)2004-10-212006-05-04Dirk De RidderNew stimulation design for neuromodulation
US7734340B2 (en)2004-10-212010-06-08Advanced Neuromodulation Systems, Inc.Stimulation design for neuromodulation
WO2006045251A1 (en)2004-10-292006-05-04Lam Philip Y TNose mask
US20060135886A1 (en)2004-12-022006-06-22Biotronik Crm Patent AgDevice for determining thoracic impedance
US20060150979A1 (en)2004-12-082006-07-13Ventus Medical, Inc.Nasal respiratory devices
WO2006063339A2 (en)2004-12-082006-06-15Ventus Medical, Inc.Respiratory devices and methods of use
US20070295338A1 (en)2004-12-082007-12-27Ventus Medical, Inc.Nasal respiratory devices for positive end-expiratory pressure
US20060150978A1 (en)2004-12-082006-07-13Ventus Medical, Inc.Methods of treating respiratory disorders
US20060144398A1 (en)2004-12-082006-07-06Rajiv DoshiRespiratory devices
US7561922B2 (en)2004-12-222009-07-14Biocontrol Medical Ltd.Construction of electrode assembly for nerve control
US20060136024A1 (en)2004-12-222006-06-22Biocontrol Medical Ltd.Construction of electrode assembly for nerve control
US20060167497A1 (en)2005-01-272006-07-27Cyberonics, Inc.Implantable medical device having multiple electrode/sensor capability and stimulation based on sensed intrinsic activity
US20060184204A1 (en)2005-02-112006-08-17Advanced Bionics CorporationImplantable microstimulator having a separate battery unit and methods of use thereof
US20100137931A1 (en)2005-02-282010-06-03Hopper Donald LImplantable Cardiac Device With Dyspnea Measurement
US7805195B2 (en)2005-03-242010-09-28Vanderbilt UniversityRespiratory triggered, bilateral laryngeal stimulator to restore normal ventilation in vocal fold paralysis
US20060282127A1 (en)2005-03-242006-12-14Vanderbilt UniversityRespiratory triggered, bilateral laryngeal stimulator to restore normal ventilation in vocal fold paralysis
US20100131029A1 (en)2005-03-312010-05-27Case Western Reserve UniversityMethod of treating obstructive sleep apnea using electrical nerve stimulation
US20060224211A1 (en)2005-03-312006-10-05Durand Dominique MMethod of treating obstructive sleep apnea using electrical nerve stimulation
US7680538B2 (en)2005-03-312010-03-16Case Western Reserve UniversityMethod of treating obstructive sleep apnea using electrical nerve stimulation
US20060241708A1 (en)2005-04-222006-10-26Willem BouteMultiple sensors for sleep apnea with probability indication for sleep diagnosis and means for automatic activation of alert or therapy
US20060241506A1 (en)2005-04-252006-10-26Melker Richard JMethod and apparatus for diagnosing respiratory disorders and determining the degree of exacerbations
US7785262B2 (en)2005-04-252010-08-31University Of Florida Research Foundation, Inc.Method and apparatus for diagnosing respiratory disorders and determining the degree of exacerbations
US20060264777A1 (en)2005-04-292006-11-23Medtronic, Inc.Event-based lead impedance monitoring
US20060259079A1 (en)2005-04-302006-11-16Medtronic, Inc.Impedance-based stimulation adjustment
US7734348B2 (en)2005-05-102010-06-08Cardiac Pacemakers, Inc.System with left/right pulmonary artery electrodes
US7765000B2 (en)2005-05-102010-07-27Cardiac Pacemakers, Inc.Neural stimulation system with pulmonary artery lead
US20070227542A1 (en)2005-05-172007-10-04Boris KashmakovNose Filter
US20060271137A1 (en)2005-05-252006-11-30The Cleveland Clinic FoundationApparatus and system to stimulate a nerve
US20060271118A1 (en)2005-05-252006-11-30Cardiac Pacemakers, Inc.Implantable neural stimulator with mode switching
US20060266369A1 (en)2005-05-272006-11-30Prospex Medical Ii, Inc.Devices and methods for treating sleep disorders
JP2007021156A (en)2005-07-192007-02-01Isao MiyagawaTool for preventing invasion of pollen in nose
US20070021785A1 (en)2005-07-212007-01-25Cyberonics, Inc.Safe-mode implantable medical devices
US20070027482A1 (en)2005-07-272007-02-01Cyberonics, Inc.Cranial nerve stimulation to treat a vocal cord disorder
US20070043411A1 (en)2005-08-172007-02-22Enteromedics Inc.Neural electrode
US7822486B2 (en)2005-08-172010-10-26Enteromedics Inc.Custom sized neural electrodes
US20100228133A1 (en)2005-09-162010-09-09Averina Viktoria ASystem and Method for Generating a Trend Parameter Based on Respiration Rate Distribution
US7128717B1 (en)2005-09-292006-10-31Washington UniversityMethod for determining airway obstruction
US20080099029A1 (en)2005-10-072008-05-01Lamberg Steven BIntraoral mandibular advancement device for treatment of sleep disorders
US20070125379A1 (en)2005-12-022007-06-07Brian PierroNasal continuous positive airway pressure device and system
US7596414B2 (en)2005-12-052009-09-29Boston Scientific Neuromodulation CorporationCuff electrode arrangement for nerve stimulation and methods of treating disorders
US7662105B2 (en)2005-12-142010-02-16Cardiac Pacemakers, Inc.Systems and methods for determining respiration metrics
US7797050B2 (en)2005-12-282010-09-14Cardiac Pacemakers, Inc.Neural stimulator to treat sleep disordered breathing
US20070150006A1 (en)*2005-12-282007-06-28Imad LibbusNeural stimulator to treat sleep disordered breathing
US7672728B2 (en)2005-12-282010-03-02Cardiac Pacemakers, Inc.Neural stimulator to treat sleep disordered breathing
US20070175478A1 (en)2006-02-012007-08-02Brunst Robert FNasal air purifier
US7725195B2 (en)2006-02-162010-05-25Imthera Medical, Inc.RFID-based apparatus, system, and method for therapeutic treatment of obstructive sleep apnea
US7697968B2 (en)2006-03-282010-04-13Kent MooreSystem and method of predicting efficacy of tongue-base therapies
US20070239243A1 (en)2006-03-302007-10-11Advanced Bionics CorporationElectrode contact configurations for cuff leads
US20070282410A1 (en)2006-04-282007-12-06Cross Thomas E JrImplantable medical lead assemblies with improved flexibility and extensibility and having a substantially two-dimensional nature
US7515968B2 (en)2006-04-282009-04-07Medtronic, Inc.Assembly method for spinal cord stimulation lead
EP1854494A1 (en)2006-05-122007-11-14Intersurgical AGImprovements Relating to Respiratory Masks
US20070277832A1 (en)2006-05-232007-12-06Ventus Medical, Inc.Nasal respiratory devices
WO2007134458A1 (en)2006-05-232007-11-29Jean-Pierre RobitailleValved nasal cannula
US20070283962A1 (en)2006-06-072007-12-13Ventus Medical, Inc.Layered nasal devices
US20080041373A1 (en)2006-06-072008-02-21Ventus Medical, Inc.Nasal devices
US20070283692A1 (en)2006-06-092007-12-13Shimano Inc.Bicycle hydraulic brake accentuate device
US20080027480A1 (en)2006-06-292008-01-31Aspire Medical, Inc.Methods and devices for rhinoplasty and treating internal valve stenosis
US7660632B2 (en)2006-06-302010-02-09Ric Investments, LlcMethod and apparatus for hypoglossal nerve stimulation
US20100100150A1 (en)2006-06-302010-04-22Ric Investments, LlcMethod and apparatus for hypoglossal nerve stimulation
US20080027502A1 (en)2006-07-282008-01-31Ransom Scott ADynamic Sampling
US20100241207A1 (en)2006-08-142010-09-23Henry BlugerImplantable Medical Cuff with Electrode Array
US20100047376A1 (en)2006-08-292010-02-25Marc-Olivier ImbeauNerve cuff injection mold and method of making a nerve cuff
US20100016749A1 (en)2006-09-192010-01-21Victhom Human Bionics, Inc.Method and System for the Monitoring of Respiratory Acitivity and for the Treatment of Breathing Disorders Such as Sleep Apnea
WO2008046190A1 (en)2006-09-192008-04-24Victhom Human Bionics Inc.Method and system for the monitoring of respiratory activity and for the treatment of breathing disorders such as sleep apnea
US20100076536A1 (en)2006-09-222010-03-25Koninklijke Philips Electronics N.V.Implantable multi-electrode device
US8249723B2 (en)2006-09-272012-08-21Huntington Medical Research InstitutesApparatus and method for treating obstructive sleep apnea
US8639354B2 (en)2006-10-132014-01-28Cyberonics, Inc.Obstructive sleep apnea treatment devices, systems and methods
US7809442B2 (en)2006-10-132010-10-05Apnex Medical, Inc.Obstructive sleep apnea treatment devices, systems and methods
US20110071591A1 (en)2006-10-132011-03-24Apnex Medical, Inc.Obstructive Sleep Apnea Treatment Devices, Systems and Methods
US8626304B2 (en)2006-10-132014-01-07Cyberonics, Inc.Obstructive sleep apnea treatment devices, systems and methods
US8498712B2 (en)2006-10-132013-07-30Apnex Medical, Inc.Obstructive sleep apnea treatment devices, systems and methods
US8428727B2 (en)2006-10-132013-04-23Apnex Medical, Inc.Obstructive sleep apnea treatment devices, systems and methods
US8311645B2 (en)2006-10-132012-11-13Apnex Medical, Inc.Obstructive sleep apnea treatment devices, systems and methods
US8744589B2 (en)2006-10-132014-06-03Cyberonics, Inc.Obstructive sleep apnea treatment devices, systems and methods
US9186511B2 (en)2006-10-132015-11-17Cyberonics, Inc.Obstructive sleep apnea treatment devices, systems and methods
US8718783B2 (en)2006-10-132014-05-06Cyberonics, Inc.Obstructive sleep apnea treatment devices, systems and methods
US20080103407A1 (en)2006-10-132008-05-01Apnex Medical, Inc.Obstructive sleep apnea treatment devices, systems and methods
US20080103545A1 (en)2006-10-132008-05-01Apnex Medical, Inc.Obstructive sleep apnea treatment devices, systems and methods
US20080147142A1 (en)*2006-12-152008-06-19Testerman Roy LMethod and apparatus for assisting deglutition
US20080163875A1 (en)2006-12-152008-07-105I Sciences, Inc.Device and method for opening an airway
US7787959B1 (en)2006-12-222010-08-31Pacesetter, Inc.Mechanism and method of attaching a stimulation and/or sensing electrode to a nerve
US20080183254A1 (en)2007-01-302008-07-31Cardiac Pacemakers, Inc.Dual spiral lead configurations
US7751880B1 (en)2007-02-122010-07-06Pacesetter, Inc.Shielded electrode assembly for effective nerve sensing and stimulation
US7758384B2 (en)2007-02-262010-07-20Medtronic, Inc.Implantable bifurcated neurostimulator adapters
US20100257729A1 (en)2007-02-262010-10-14Medtronic, IncImplantable bifurcated neurostimulator adapters
US7725198B2 (en)2007-04-302010-05-25Medtronic, Inc.Implantable medical lead assemblies with delivery tether
US7634315B2 (en)2007-05-312009-12-15Pacesetter, Inc.Techniques to monitor and trend nerve damage and recovery
US20090044814A1 (en)2007-06-182009-02-19Koninklijke Philips Electronics N.V.Implantable devices, systems, and methods for maintaining desired orientations in targeted tissue regions
US7630771B2 (en)2007-06-252009-12-08Microtransponder, Inc.Grooved electrode and wireless microtransponder system
US20090270707A1 (en)2008-04-232009-10-29Medtronic, Inc.Sensor Assemblies for Implantable Medical Electrical Leads
US20090276024A1 (en)2008-05-022009-11-05Bonde Eric HSelf expanding electrode cuff
US20100137949A1 (en)2008-05-272010-06-03The Cleveland Clinic FoundationBifurcated electrical lead and method of use
US20090318986A1 (en)2008-06-202009-12-24Alo Kenneth MSystems, Methods and Apparatus for Treating Cardiac Dysfunction with Neurostimulation
US20090326408A1 (en)2008-06-302009-12-31Loell Boyce MoonProviding Impedance Plethysmography Electrodes
US20100036285A1 (en)2008-08-062010-02-11Assaf GovariSingle-axis sensors on flexible backbone
US20100094379A1 (en)2008-10-092010-04-15Imthera Medical, Inc.Method of Stimulating a Hypoglossal Nerve for Controlling the Position of a Patient's Tongue
US20100125310A1 (en)2008-11-182010-05-20Willard WilsonMethod and Device For the Detection, Identification and Treatment of Sleep Apnea/Hypopnea
US20100174341A1 (en)2008-12-312010-07-08Bolea Stephen LObstructive Sleep Apnea Treatment Devices, Systems and Methods
US20110093032A1 (en)2009-08-052011-04-21Ndi Medical, LlcSystems and methods for maintaining airway patency
US20120192874A1 (en)2011-01-282012-08-02Apnex Medical, Inc.Obstructive sleep apnea treatment devices, systems and methods
US8386046B2 (en)2011-01-282013-02-26Apnex Medical, Inc.Screening devices and methods for obstructive sleep apnea therapy
US8855771B2 (en)2011-01-282014-10-07Cyberonics, Inc.Screening devices and methods for obstructive sleep apnea therapy
US20130085546A1 (en)2011-05-122013-04-04Stephen BoleaDevices and methods for sleep apnea treatment

Non-Patent Citations (27)

* Cited by examiner, † Cited by third party
Title
Aziz, L.and Ejnell, H. "Obstructive Sleep Apnea Caused by Bilateral Vocal Fold Paralysis." Ear Nose Throat J. Apr. 2003; 82(4): 326-7. Abstract.*
Campbell et al., "Nasal Continuous positive airway pressure from high flow cannula versus Infant Flow for preterm infants," Journal of Perinatology, Jul. 2006, pp. 546-549, vol. 26 (9), Nature Publishing Group.
De Almeida et al., "Nasal pressure recordings to detect obstructive sleep apnea," Sleep and Breathing, Feb. 25, 2006, pp. 62-69, vol. 10 (2), Springer Heidelberg.
European Search Report for Patent Application No. 16162666, dated Jul. 8, 2016, 7 pages.
European Search Report issued in corresponding European Application No. 121 637 91 on Jun. 25, 2012, 3 pages.
Extended European Search Report for EP Application No. 15192695.3 dated Mar. 2, 2016, 7 pages.
Extended Search Report on European application No. 19151866 dated May 22, 2019. 7 pages.
Ferguson et al., "Effect of Mandibular and Tongue Protrusion on Upper Airway Size During Wakefulness," American Journal of Respiratory and Critical Care Medicine, 1997, pp. 1748-1754, vol. 155.
Goding Jr. et al., "Relief of Upper Airway Obstruction With Hypoglossal Nerve Stimulation in the Canine," The Laryngoscope, Feb. 1998, pp. 162-169, vol. 108, Lippincott-Raven Publishers, U.S.A.
Huang et al. "Dilation of the oropharynx via selective stimulation of the hypoglossal nerve." J. Neural Eng. 2005; 2:73-80.
Isono et al., "Interaction of cross-sectional area, driving pressure, and airflow of passive velopharynx," American Physiological Society, 1997, pp. 851-859, vol. 83.
Kirkness et al., "Nasal airflow dynamics: mechanisms and responses associated with an external nasal dilator strip," University of Western Sydney, T.C. Amis School of Science, Department of Respiratory Medicine, Westmead Hospital and University of Sydney, Westmead, Australia, 2000.
Mahadevia et al., "Effects of expiratory positive airway pressure on sleep-induced respiratory abnormalities in patients with hypersomnia-sleep apnea syndrome," Am. Rev. Respir. Dis., Feb. 1983, vol. 128, pp. 708-711.
Noseda et al., "Compliance with nasal continuous positive airway pressure assessed with a pressure monitor: pattern of use and influence of sleep habits," Chest Clinics and Sleep Laboratories, Hôpitaux Erasme et Brugmann, Université Libre de Bruxelles, Brussels, Belgium, 2000, vol. 94, pp. 76-81.
Oliven et al., "Effect of genioglossus contraction on pharyngeal lumen and airflow in sleep apnoea patients," European Respiratory Journal, 2007, pp. 748-758, vol. 30, No. 4.
Paquereau et al., "Positive pressure titration in the treatment of obstructive sleep apnea syndrome using continuous airway positive pressure," Revue Des Maladies Respiratoires, Apr. 2000, pp. 459-465, vol. 17 (2), Masson Editeur, Abstract.
Partial European Search Report dated Aug. 19, 2009, issued in corresponding European Patent Application No. 09161958.5 (4 pages).
Response to the Notice of Opposition for Opposition against patent EP 2 116 274 (Application No. 09 161 958.5) dated Dec. 2, 2013 (30 pages).
Sahin et al., "Chronic recordings of hypoglossal nerve activity in a dog model of upper airway obstruction," Journal of Applied Physiology 87(6), 1999, The American Physiological Society, pp. 2197-2206.
Saslow et al., "Work of breathing using high-flow nasal cannula in preterm infants," Journal of Perinatology, May 11, 2006, pp. 476-480, vol. 26 (8), Nature Publishing Group.
Schwartz et al. "Therapeutic Electrical Stimulation of the Hypoglossal Nerve in Obstructive Sleep Apnea." Arch Otolaryngol Head Neck Surg/vol. 127, Oct. 2001 (8 pages).
Spence et al., "High-flow nasal cannula as a device to provide continuous positive airway pressure in infants," Journal of Perinatology, Dec. 2007, pp. 772-775, vol. 27 (12), Nature Publishing Group.
Statement of Grounds filed in Opposition of EP Patent No. 2116274 dated Jul. 25, 2012 (32 pages).
Stern et al. "Obstructive sleep apnea following treatment of head and neck cancer", Ear, Nose, and Throat Journal, Feb. 2007, vol. 86, No. 2, pp. 101-103.
Tiran et al., "An Improved Device for Posterior Rhinomanometry to Measure Nasal Resistance," Journal of Biomechnical Engineering, Nov. 2005, vol. 127, pp. 994-997.
Trevisanuto et al., "A new device for administration of continuous positive airway pressure in preterm infants: comparison with a standard nasal CPAP continuous positive airway pressure system," Intensive Care Medicine, Apr. 2005, pp. 859-864, vol. 31 (6), Springer-Verlag.
Verse et al., "New developments in the therapy of obstructive sleep apnea," European Archives of Oto-Rhino-Laryngology, Jan. 2001, pp. 31-37, vol. 258 (1), Springer-Verlag.

Cited By (1)

* Cited by examiner, † Cited by third party
Publication numberPriority datePublication dateAssigneeTitle
US12226223B2 (en)2011-09-062025-02-18Resmed Sensor Technologies LimitedMulti-modal sleep system

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