US20060178617A1

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Publication number: US20060178617A1
Application number: US11/402,158
Authority: US
Inventors: H. Adams; Brian Brockway; Perry Mills
Original assignee: Transoma Medical Inc
Current assignee: Data Sciences International Inc
Priority date: 2002-09-17
Filing date: 2006-04-10
Publication date: 2006-08-10
Also published as: US20040054352A1; US7070591B2; US20070049806A1

Abstract

A combined vascular access port and physiologic parameter monitoring device. The vascular access port and the monitoring device may be connected by a cooperative geometry. The vascular access port and the monitoring device may be implanted at the same time and in the same anatomical location (e.g., subcutaneous pocket). The monitoring device may include a telemetry unit that transmits physiological measurement data to a local data collection system (e.g., carried by the patient or located in the patient's home), which may re-transmit the data to a remote data collection system (e.g., located at a physician's office or clinic) via a suitable communication link.

Description

CROSS-REFERENCES TO RELATED APPLICATIONS

This application is a continuation of U.S. patent application Ser. No. 10/246,348, filed Sep. 17, 2002, the entire disclosure of which is incorporated herein by reference.

BACKGROUND OF THE INVENTION

The present invention generally relates to vascular access ports. In particular, the present invention relates to vascular access ports having associated physiological sensors.

Implantable vascular access ports (VAP) are used extensively in the medical field when recurrent infusions of therapeutic agents into a patient's circulatory system are required over extended periods of time. Such VAPs generally include a housing containing a reservoir and septum, with a catheter extending from the housing. The VAP housing is implanted in a subcutaneous pocket at an accessible location such as the arm, and the catheter extends from the housing to a remote vascular location to provide convenient, repeatable access to the patient's venous or arterial system in the body. In the subcutaneous pocket, the septum of the VAP may be pierced by a needle that is coupled via appropriate tubing to a therapeutic agent source in an intravenous bag or infusion pump, for example, so that the therapeutic agents may be administered. Such a vascular access system may be used in the home or other outpatient settings, as well as inpatient hospital settings.

When infusing therapeutic agents, it is important to monitor certain patient physiological parameters in order to assess if the therapeutic agent is having the desired benefit and/or is causing detrimental side effects. For example, home infusions of antibiotics are often prescribed for patients suffering from aggressive bacterial infections. These infusions are administered for weeks and then terminated if no apparent clinical symptoms exist. In some instances, however, patients remain infected even though no symptoms exist. The residual infection often manifests itself as random temperature spikes lasting for tens of minutes (known as infection rebound or breakthrough) and the patient may or may not be aware of its existence. As such, patient temperature should be monitored because such temperature spikes should signal the attending physician to change antibiotics. As another example, infused inotropic or antihypertensive drugs require patient blood pressure monitoring because of possible hypo or hypertension side effects that may be life threatening.

Conventional options for monitoring temperature include oral, rectal, ear or skin type temperature measurement devices. Blood pressure monitoring typically includes a blood pressure cuff device. In addition to inconvenience, these devices are not desirable due to lack of continuous monitoring and lack of patient compliance in outpatient settings. For example, because temperature spikes only last a brief period of time as discussed above, periodic monitoring may not catch the temperature spike. Furthermore, because these monitoring devices require patient use, and because typical patients do not have professional health care training, the devices are susceptible to incorrect usage, potentially resulting in erroneous measurements.

Thus, there is a need for a monitoring device that is convenient to the patient as well as the physician, provides the potential for continuous monitoring, and reduces patient non-compliance.

BRIEF SUMMARY OF THE INVENTION

To address this need and others, the present invention provides, in one exemplary embodiment, a vascular access port and physiologic parameter (e.g., temperature, blood pressure, etc.) monitoring device that may be inter-connected by a cooperative geometry. The inter-connected vascular access port and monitoring device may be implanted at the same time and in the same anatomical location (e.g., subcutaneous pocket). The monitoring device may include a telemetry unit that transmits physiological measurement data to a local data collection system (e.g., carried by the patient or located in the patient's home), which may re-transmit the data to a remote data collection system (e.g., located at a physician's office or clinic) via a suitable communication link.

Because the combined vascular access port and monitoring device may be implanted at the same time and in the same anatomical location, it is very convenient for the physician and procedurally cost effective. Also, because the monitoring device does not require patient involvement for effective use, it is not as susceptible to patient non-compliance as prior art monitoring devices. In addition, because the monitoring device permits continuous feedback; it is possible to detect patient symptoms that may occur infrequently and for short periods of time. Furthermore, because the monitoring device permits multiple measurements over a long period of time, it is possible to improve accuracy of measurements that lack repeatability by averaging multiple measurements over a period of time.

BRIEF DESCRIPTION OF THE DRAWINGS

FIG. 1 is a schematic plan view of a vascular access port and physiological monitoring system in accordance with a generic embodiment of the present invention;

FIG. 2A is a schematic view of a vascular access port and physiological monitoring apparatus connected together by a connector element;

FIG. 2B is a schematic view of a vascular access port and physiological monitoring apparatus connected together by a cooperative geometry;

FIGS. 3A-3D are schematic illustrations of various connector element designs for use in the vascular access port and physiological monitoring apparatus illustrated inFIG. 2A;

FIG. 4 is a schematic illustration of a vascular access port for use in the present invention;

FIG. 5 is a schematic illustration of a physiological monitoring apparatus for use in the present invention;

FIG. 6 is a perspective view of a vascular access port and physiological monitoring apparatus in accordance with a specific embodiment of the present invention;

FIG. 7 is an exploded perspective view of the vascular access port and physiological monitoring apparatus illustrated inFIG. 6;

FIG. 8 is a block diagram of the electronics of a physiological monitoring apparatus and associated transceiver for use with the embodiment illustrated inFIG. 6;

FIG. 9A is a perspective view of a pressure transmission catheter having an antenna for use with the physiological monitoring apparatus illustrated inFIG. 6;

FIG. 9B is an end view of the pressure transmission catheter and antenna illustrated inFIG. 9A;

FIG. 10A is an end view of an alternative embodiment of a pressure transmission catheter having an antenna;

FIG. 10B is an end view of another alternative embodiment of a pressure transmission catheter having an antenna;

FIG. 11A is a perspective view of a vascular access port and physiological monitoring apparatus having an alternative connector element;

FIG. 11B is a perspective view of a vascular access port and physiological monitoring apparatus having another alternative connector element;

FIG. 11C is a perspective view of a vascular access port and physiological monitoring apparatus connected together by a cooperative geometry;

FIG. 12 is an exploded perspective view of an alternative embodiment of a vascular access port and physiological monitoring apparatus connected together by a common or integral housing; and

FIG. 13 is an exploded perspective view of another alternative embodiment of a vascular access port and physiological monitoring apparatus connected together by a common or integral housing.

DETAILED DESCRIPTION OF THE INVENTION

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.

With reference toFIG. 1, a schematic plan view of a generic system including a vascular access port (VAP)100 and physiological monitoring apparatus (PMA)200 is shown. The system may be used to deliver therapeutic agents via theVAP100 while monitoring thepatient10 with thePMA200. Based on the patient's condition as measured by thePMA200, the therapeutic regimen (e.g., dose, delivery rate, delivery schedule, etc. of therapeutic agent administered via the VAP100) may be changed as needed. For example, if the patient10 adversely reacts to the therapeutic agent delivered via theVAP100 as measured by thePMA200, the dose or delivery rate may be decreased or even terminated to reduce or eliminate the adverse effect. Also by way of example, if thepatient10 is not responding to the therapeutic agent delivered via theVAP100 as measured by thePMA200, the dose or delivery rate may be increased to establish the desired therapeutic effect. Further by way of example, if thepatient10 demonstrates a need for therapeutic intervention as measured by thePMA200, the administration of therapeutic agent may be initiated via theVAP100.

In these and other modes of operation, thePMA200 provides feedback as to the condition of the patient10 as indicated by measuring one or more physiological parameters such as blood pressure (arterial, venous, pulse pressure, etc.), temperature, ECG, blood flow velocity, impedance, blood gas levels, blood gas constituents, etc., or combinations thereof. The feedback provided by thePMA200 may be used to automatically or manually modify the therapeutic regimen (i.e., delivery parameters of the therapeutic agent administered via the VAP100) as described above. Alternatively, thePMA200 may provide measurement data indicative of the patient's condition independent of the therapy administered via theVAP100.

In addition to theVAP100 andPMA200, the generic system illustrated inFIG. 1 may include a home (local) data collection system (HDCS)300 which is operably connected to thePMA200 viacommunication link400, in addition to a physician (remote) data collection system (PDCS)500 which is operably connected to theHDCS300 viacommunication link600.Communication link400 may comprise a direct connection (e.g., hardwired transdermal, ohmic, galvanic or body bus) or an indirect (wireless) connection (e.g., radiofrequency, ultrasonic, or infrared transmission). By way of example, not limitation, thecommunication link400 may be provided via a conductive needle (not shown) inserted into theVAP100, wherein the needle is electrically coupled to theHDCS300 via a wired connection, and electrically coupled to thePMA200 via a conductive septum, for example. Similarly,communication link600 may comprise a direct (hardwired) or indirect (wireless) connection, optionally making use of a telecommunication system such as the Internet.

TheHDCS300 may be carried by the patient or may be located in the patient's home, and receives signal data from thePMA200 viacommunication link400. TheHDCS300 may process and store the signal data, and may optionally provide a visual display of the measured parameter and/or an audible alarm indicative of the measured parameter triggering a threshold value. Optionally, the HDCS may obtain an externally derived parameter (e.g., ambient pressure) and associate the external parameter with the signal data from thePMA200. The data collected and processed by theHDCS300 may be transferred to thePDCS500 viacommunication link600, which may be located at a physician's office or clinic. ThePDCS500 may further process and store the signal data, and may also provide a visual display of the measured parameter and/or an audible alarm indicative of the measured parameter triggering a threshold value.

Based on information provided byHDCS300, the patient10 or the patient's care taker may manually alter the therapeutic regimen as described above. Similarly, based on information provided byPDCS500, the physician or health care provider may contact (viaHDCS300, for example) and instruct the patient10 or the patient's care taker to manually alter the therapeutic regimen as described above. Alternatively, if the therapeutic agent is delivered to theVAP100 by an automated infusion pump or the like, theHDCS300 may be operably coupled to the infusion pump and may be programmed to modify the delivery parameters as a function of the physiological parameter measured by thePMA200 and/or as a function of instructions provided byPDCS500. Further aspects of the function and use ofHDCS300 andPDCS500 may be found in U.S. patent application Ser. No. 10/077,566, filed Feb. 15, 2002, entitled DEVICES, SYSTEMS AND METHODS FOR ENDOCARDIAL PRESSURE MEASUREMENT, the entire disclosure of which is incorporated herein by reference.

With reference toFIGS. 1, 2A,2B, and4, theVAP100 is shown schematically and may comprise a variety of vascular access port (single or dual port) designs known to those skilled in the art, with certain modification as described in more detail hereinafter. In the illustrated embodiment, theVAP100 includes aportal housing102 and an elongatetubular infusion catheter104 extending therefrom. An internal reservoir110 (visible inFIG. 4) is contained within thehousing102. Thehousing102 includes two openings, both of which are in fluid communication with and provide access to theinternal reservoir110. A side opening in thehousing102 permits passage of theinfusion catheter104 which is in fluid communication with theinternal reservoir110. The side opening in thehousing102 may contain a catheter connector and/or strain relief108 (visible inFIGS. 2A, 2B and4). A top opening in thehousing102 contains a self-sealingseptum106 through which a hypodermic or infusion needle may be removably inserted into theinternal reservoir110 for the delivery of therapeutic agents. An example of asuitable VAP100, with some modification, is disclosed in U.S. Pat. No. 5,387,192 to Glantz et al., the entire disclosure of which is incorporated herein by reference. As an option, theVAP100 may incorporate a needle detector device as described in U.S. patent application Ser. No. 10/246,324, entitled VASCULAR ACCESS PORT WITH NEEDLE DETECTOR, filed on even date herewith, the entire disclosure of which is hereby incorporated by reference.

With reference toFIGS. 1, 2A,2B, and5, thePMA200 is shown schematically and may comprise a variety of implantable sensor devices known to those skilled in the art, with certain modification as described in more detail hereinafter. Examples of implantable devices that measure blood pressure are described in U.S. Pat. No. 4,846,191 to Brockway et al., U.S. Pat. No. 6,033,366 to Brockway et al., U.S. Pat. No. 6,296,615 to Brockway et al., and PCT Publication WO 00/16686 to Brockway et al., the entire disclosures of which are incorporated herein by reference. Other implantable sensor devices that measure temperature, ECG, blood constituents, etc., may be implemented as well. An example of an implantable device with a temperature sensor is described in U.S. Pat. No. 5,535,752 to Halperin et al., the entire disclosure of which is incorporated herein by reference. An example of an implantable device with temperature, pH and pressure sensing capabilities is disclosed in U.S. Pat. No. 6,285,897 to Kilcoyne et al., the entire disclosure of which is incorporated herein by reference. An example of an implantable device with blood flow velocity measuring capabilities is disclosed in U.S. Pat. No. 5,522,394 to Zurbrugg, the entire disclosure of which is incorporated herein by reference. An example of an implantable device with blood constituent (e.g., blood glucose, blood gas) measuring capabilities is disclosed in U.S. Pat. No. 6,122,536 to Sun et al., the entire disclosure of which is incorporated herein by reference. The sensor components (transducer and pressure transmission catheter) of thePMA200 may be replaced by the sensor components of the implantable sensor devices described in the patents identified above. In some instances, the transducer may be located on thePMA housing202, or on a catheter or lead extending therefrom. In other instances, the transducer may be located on theVAP housing102 or thecatheter104 extending therefrom.

For purposes of illustration, the present invention is described herein primarily with reference to embodiments utilizing aPMA200 that measures blood pressure as described in Brockway et al. '191. To this end, in the embodiment illustrated inFIGS. 1, 2A,2B, and5, thePMA200 comprises a blood pressure measuring device including asensor housing202 with a pressure transmission catheter (PTC)204 extending therefrom. ThePMA200 also includes a pressure transducer andelectronics module210, atelemetry unit220 and a power supply230 (e.g., battery, external power source with transdermal connection, etc.) contained in housing202 (visible inFIG. 5).

Thehousing202 protects the pressure transducer and theelectronics module210, thetelemetry unit220, and thepower supply230 from the harsh environment of the human body. Thehousing202 may be fabricated of a suitable biocompatible material such as titanium or ceramic and may be hermetically sealed. If metallic, the outer surface of thehousing202 may serve as an electrocardiogram (ECG) sensing electrode. The housing may include one or more rings (not shown) and/or a mesh fabric (not shown) disposed thereon for attachment to bodily tissue in the subcutaneous pocket.

ThePTC204 refers pressure from the pressure measurement site to the pressure transducer andelectronics module210 located inside thesensor housing202. ThePTC204 may comprise a tubular structure with a liquid-filled lumen extending therethrough to a distal opening or port. The proximal end of thePTC204 is connected to the pressure transducer via a nipple tube, thus establishing a fluid path from the pressure transducer to the distal end of thePTC204. A barrier such as a viscous or movable plug and/or membrane may be disposed in the distal opening of thePTC204 to isolate the liquid-filled lumen of thePTC204 from bodily fluids, without impeding pressure transmission therethrough.

As an alternative, thePTC204 of thePMA200 and theinfusion catheter104 of theVAP100 may be combined into one dual lumen tube, wherein thePMA200 measures blood pressure and theVAP100 delivers therapeutic agent in the same blood vessel. As another alternative, thePTC204 theinfusion catheter104 may be combined into a single lumen tube, wherein a valve is used to alternatively provide fluid communication between thePMA200 and the single lumen catheter to measure blood pressure, and provide fluid communication between theVAP100 and the single lumen catheter to deliver therapeutic agent. In addition or in the alternative, thePMA200 may be used to measure fluid flow and/or pressure in theVAP100 during infusion, in addition to measuring a physiological parameter.

The pressure transducer andelectronics module210 may be the same or similar to those described in U.S. Pat. Nos. 4,846,191, 6,033,366, 6,296,615 or PCT Publication WO 00/16686, all to Brockway et al. The electronics module provides excitation to the pressure transducer, amplifies the pressure signal, and may digitally code the pressure information for communication to thetelemetry unit220. The electronics module may also provide for temperature compensation of the pressure transducer and provide a calibrated pressure signal.

Thetelemetry unit220 includes telemetry electronics, which may be the same or similar to those described in U.S. Pat. Nos. 4,846,191, 6,033,366, 6,296,615 or PCT Publication WO 00/16686, all to Brockway et al. Thetelemetry unit220, receives a physiological parameter (e.g., pressure) signal from the pressure transducer andelectronics module210, and transmits the data signal to theHDCS300 viacommunication link400. In addition or in the alternative, thetelemetry unit220 may include memory interrogatable by theHDCS300.Communication link400 may comprise a direct connection (e.g., hardwired transdermal, ohmic, galvanic or body bus) or an indirect (wireless) connection (e.g., radiofrequency, ultrasonic, or infrared transmission). For wireless RF transmission, a telemetry coil or antenna may be provided in thehousing202, or an antenna may be provided in thePTC204 as described in more detail hereinafter.

The pressure as measured by thePMA200 is influenced by external pressure changes (i.e., barometric pressure) and is preferably corrected to avoid inaccuracies and/or possible misinterpretation of pressure data. Barometric pressure can change significantly when a weather front moves through the area where the patient resides, when the patient is riding up an elevator in a tall building or traveling in mountainous areas where changes in elevation are frequent and significant. Thus, the present invention provides a number of different pressure correction schemes as described herein.

One general approach is to take barometric pressure measurements simultaneously with measurements taken by thePMA200, and subtract the barometric reading from the internal pressure measurement. For example, theHDCS300 may take a barometric pressure reading and subtract the barometric pressure measurement from the pressure measurement transmitted bytelemetry unit220 of thePMA200.

For example, a barometric pressure monitor (BPM) may be located external to the body and measure barometric pressure at times specified by a controller. Measurements obtained by the BPM are representative of the barometric pressure to which the body of the patient is exposed. The BPM may be a small device attached to a belt, worn on the neck as a pendant, on the wrist like a watch, or placed in a purse or briefcase. The BPM may be incorporated into theHDCS300, for example.

At some time, e.g. the first measurement obtained after the BPM is powered on, the absolute value of barometric pressure is stored in the memory of a computing device, which may be incorporated into the BPM, for example. The absolute value of barometric pressure is stored in the memory along with a time stamp (e.g. year, month, day, hour, minute and second). From then on, each subsequent barometric pressure measurement is compared to the stored measurement and evaluated to determine if the difference between that measurement and the stored measurement exceeds a predetermined threshold (e.g. 0.5 mmHg). If the difference is less than the threshold, no further action is taken on that measurement. If the difference is greater than or equal to the threshold, then that value is saved in memory along with a time stamp. If a chronic time series is collected from the patient, the memory of the computing device in the BPM contains barometric pressure values at each point in time where the pressure changed significantly (significant as determined by the preset value).

With this approach, pressure measurements taken by thePMA200 are made with respect to a specific reference pressure, normally to a vacuum. Pressure measurements are recorded into memory in thePMA200. Measurements are stored in a way that allows the date and time of the recording to be established. At various times, the pressure measurements recorded in thePMA200 are transferred to an external combining device (CD) through means of a wireless link. The CD may also be incorporated into theHDCS300, for example, and the BPM also has the ability to transfer measurements to the CD. This transfer can be made through a hard link (e.g., electrically conductive wires or fiber optics) if the BPM and CD are in the same unit such asHDCS300, or via a wireless link (e.g., RF transmission) if the BPM and CD are remote from each other. Once data from both thePMA200 and the BPM are transferred to the CD, the CD can correct the measurements obtained from thePMA200 for barometric pressure. Knowing the barometric pressure measurements at the starting time and at each point thereafter when pressure changes by a significant amount, it is possible to know the barometric pressure at any time up until the date and time of the last value recorded in memory. Correction of a measurement from thePMA200 for barometric pressure can be achieved by subtracting the barometric pressure measurement reconstructed at that time point, or by mathematically manipulating the two time series to achieve a result equivalent to subtraction.

A variation of this approach is to record corrected measurements within thePMA200. In some cases it is useful to have the corrected pressure measurements available within thePMA200, such as when thePMA200 is in communication with a device that is providing therapeutic effect, such as an infusion pump, pacemaker or defibrillator, and is relying on accurate pressure measurements to adjust the therapy parameters. Such a therapeutic device may be implanted or external (e.g., a drug infusion pump or wearable defibrillator).

The BPM may transmit barometric pressure data to thePMA200, which subtracts the barometric measurement from the in vivo pressure measurement and utilizes or otherwise stores the corrected measurement. Alternatively, the in vivo pressure measurements may be transmitted to the BPM which corrects the pressure measurement from thePMA200 for barometric pressure and transmits the corrected pressure measurement back into thePMA200.

Alternately, the BPM may evaluate the barometric pressure measurements as they are obtained. In this alternative embodiment, the BPM would transmit the barometric pressure to thePMA200 when it is first turned on or brought into the receiving range of the BPM. Once this initial measurement is received by thePMA200, if a measurement differs from the previous value by more than a predetermined threshold, then (and only then) would the BPM transmit a barometric pressure measurement to thePMA200. ThePMA200 would then send a confirming transmission to the BPM indicating that the transmission of barometric pressure was correctly received. The BPM may continue to send the measurement at regular internals until such confirmation is received.

Another general approach is to provide a reference pressure for thePMA200. For example, a barometric reference pressure may be provided via a needle inserted into a reference septum in thePMA200 as described with reference toFIGS. 6 and 7. Alternatively, a barometric reference pressure may be provided via a needle inserted into the septum of theVAP100, which is in fluid communication with thePMA200 as described with reference toFIG. 2A.

With reference back toFIG. 1, theVAP100 is shown implanted with thehousing102 in a subcutaneous pocket and thecatheter104 inserted in a vein. Similarly, thePMA200 is shown connected to and adjacent theVAP100 in the same subcutaneous pocket, with thePTC204 disposed in an artery. Those skilled in the art will recognize that theVAP100 may be implanted in a variety of subcutaneous locations, and that theinfusion catheter104 may be inserted at a variety of venous locations with varying access and terminus sites. Similarly, those skilled in the art will recognize thatPMA200 may be implanted in a variety of subcutaneous locations, and that thePTC204 may be inserted at a variety of vascular lumens, organ cavities, interstitial spaces etc., depending on the type of sensor utilized and the type of physiological parameter measured. In addition, because some types of sensors do not require aPTC204, thePMA200 may exclude thePTC204 and simply be implanted adjacent theVAP100.

In the specific implant example shown inFIG. 1, theinfusion catheter104 of theVAP100 may be disposed in thebasilic vein24 orcephalic vein26 which converge into theauxiliary vein22. Theinfusion catheter104 may extend through theauxiliary vein22 and thesuperior vena cava20, and into the right atrium or right ventricle of theheart12. ThePTC204 of thePMA200 may be disposed in thebrachial artery18 which communicates with the left ventricle of theheart12 viaaortic arch14 andsubclavian artery16. Although the patient10 in this example is shown as a human, the present invention is equally applicable to other animals as well.

With reference toFIGS. 2A and 2B, theVAP100 andPMA200 are connected together by a cooperative connector geometry and a cooperative housing geometry, respectively. InFIG. 2A, the cooperative geometry is defined external of theport housing102 andsensor housing202. InFIG. 2B, the cooperative geometry is defined internally by one of theVAP100 andPMA200, and externally by the other. As used herein, the term cooperative geometry or geometries refers to geometries that limit relative movement along two or more orthogonal directions or axes. For example, mating geometries and interlocking geometries, whether fixed together or separable, comprises cooperative geometries.

With specific reference toFIG. 2A, theconnector element150 includes aport portion148 and asensor portion152, each of which define geometries that are cooperative. Theport portion148 of theconnector element150 may be connected to theport housing102, and may be a separate or an integral component. Similarly, thesensor portion152 of theconnector element150 may be connected to thesensor housing202, and may be a separate or an integral component.

Examples ofsuch connector elements150 with cooperative geometries are shown inFIGS. 3A-3D. InFIG. 3A, theconnector element150A defines a dove-tail interlocking geometry. InFIG. 3B, theconnector element150B defines a ball-and-socket interlocking geometry. InFIG. 3C, theconnector element150C defines a snap-fit (tapered ridge in groove) geometry. InFIG. 3D, theconnector element150D comprises a threaded shaft and bore geometry.

Connector element

150 may optionally incorporate alumen158 through which a fluid path may be established between theVAP100 and thePMA200. Thelumen158 may be used, for example, for measuring the pressure or flow rate of fluid infused throughVAP100 utilizingPMA200, for providing a reference pressure to thePMA200 via a secondary port in theVAP100, or for utilizing a common catheter for infusion and pressure measurement.

With specific reference toFIG. 2B, theport housing102 and thesensor housing202 define cooperative geometries. As shown, theVAP100 defines an external geometry which cooperates with an internal geometry of thePMA200. It is also possible to have thePMA200 define an external geometry which cooperates with an internal geometry of theVAP100. In the illustrated embodiment, thePMA200 defines a cylindrical hole orrecess206 which accommodates thecylindrical housing102 of theVAP100, in addition to theinfusion catheter104 and the catheter connector/strain relief108.

FIGS. 1-5 and the corresponding text schematically illustrate and describe generic embodiments of the present invention. Reference may be made toFIGS. 6-13 for detailed embodiments that incorporate the general principles discussed above.

With specific reference toFIG. 6, a combined vascular access port and physiological monitoring apparatus is shown generally as710. Thesystem710 includes a vascular access port (VAP)712 and physiological monitoring apparatus (PMA)714. An exploded view of the combined VAP andPMA710 is shown inFIG. 7.

A housing, comprising amating cap718 andbase720 pair, contains the internal components of both theVAP712 and PMA714. In this embodiment, thecap718 is an integrally formed component that includes the side-by-side, generally cylindrical vascularaccess port portion722 and the generally triangular-solid shapedPMA portion724. A plurality ofsuture holes726 are provided in thebase720 for securing thehousing718/720 to bodily tissue during surgical implantation thereof.

TheVAP712 includes aninfusion catheter728 that extends from theVAP housing722. Aproximal end730 of theinfusion catheter728 is connected to and is in fluid communication with areservoir754, and adistal end732 of thecatheter728 is disposed in the patient's vascular system. The therapeutic agent is delivered to theinfusion catheter728 via a needle (not shown), coupled via appropriate tubing to a therapeutic agent source in an intravenous bag or infusion pump, for example, that penetrates theinfusion septum734 and communicates withreservoir754.

The PMA714 includes a pressure transmission catheter (PTC)736 coupled at itsproximal end738 to the pressure transducer andelectronics package760 for measuring an internal body pressure. Such pressure might include, but is not limited to, arterial pressure, venous pressure, cardiac chamber pressure, intracranial pressure, intrauterine pressure, bladder pressure, or intrapleural pressure. ThePTC736 may comprise the type described in Brockway '191 or the type described in Brockway '366, for example. Apressure reference septum740 is provided that is penetrable by a needle (not shown) for providing a reference pressure, such as atmospheric pressure.

In this manner, a combined VAP andPMA710 is disclosed that allows the combined convenience of a VAP and the simultaneous ability to monitor a physiological parameter of a patient without requiring a practitioner to independently monitor the parameter. It also allows this to be accomplished in a single surgical procedure which presents virtually no additional surgical effort on behalf of the surgeon who would otherwise have implanted a VAP. It adds virtually no additional procedure time or expense either.

Although various geometries are possible, thecap718 may be generally about 25 mm in length (l), about 12 mm in width (w), and about 15 mm in height (h). Thecap718 may be formed of a titanium, titanium-plastic combination or a titanium-ceramic combination. Two access ports (holes) in thecap718, infusionseptum access port742 and pressure referenceseptum access port744, provide needle access during use to theinfusion septum734 andpressure reference septum740, respectively. In one embodiment, the septa are formed of a silicone elastomeric material. The septa are mechanically secured when thecap718 is mated to thebase720.

In the embodiment shown, thecap718 mates with the base720 by pinching anedge746 of thecap718 between awall periphery748 of thebase720 and a plurality oftabs750. The distance of thetabs750 from thewall periphery748 may be selected relative to the thickness of theedge746 of thecap718 to form a snug interference fit. Thecap718 and the base720 may further be adhesively bonded and sealed with a suitable biocompatible adhesive.

When mated, theinfusion septum734 overlays a top752 of thefluid reservoir754. In this manner, a needle may penetrate theinfusion septum734 and deliver a therapeutic agent to thefluid reservoir754. In turn, the therapeutic agent is delivered to the patient via theinfusion catheter728 which is in fluid communication with thefluid reservoir754.

Thepressure reference septum740 is secured between aclamshell structure756 of thebase720 and acurved portion758 of the cap. In this manner, it will be appreciated that atmospheric pressure (reference pressure) may be provided via a needle penetrating thepressure reference septum740 of the PMA714, which avoids the use of elaborate barometric pressure reference devices when measuring arterial or venous pressure.

ThePTC736 is connected to thebase720 via aretaining mechanism759. The pressure transducer andelectronics package760, powered bybattery source762, is coupled to thePTC736. Asubstrate764 may support theelectronics package760 and rest on thefloor766 of the base720 housing.

With reference toFIG. 8, the pressure transducer andelectronics module760 of the PMA714 may be implanted within a patient's body (shown as being to the left side of a dashedline767 representing the skin surface of the patient) and communicates, regarding measured physiological parameters, with atransceiver770 external to the patient's body (shown as being to the right side of the dashed line767).

The pressure transducer andelectronics module760 may comprise aprocessor768 having amemory772 for permanent or temporary storage of various algorithms, routines, computer executable instructions, and/or storage of the measured physiological parameter. The memory may be any well known random-access or read-only type memory, or both. A temperature input (Temp), a body pressure input (Pressure), an electrocardiogram electrode input (ECG) or other input desired to be measured by the PMA are supplied to theprocessor768 via appropriate electronic communications paths. Other inputs include, but are not limited to, blood flow, blood glucose, blood gas (e.g., oxygen saturation, CO2).

The body pressure input may be provided via thePTC736 and pressure transducer inmodule760 as described with reference toFIGS. 6 and 7. The temperature input may be received from a thermistor (not shown) mounted internally or externally to thehousing718/720. A benefit of locating the thermistor externally to the housing is to minimize temperature error induced by the therapeutic agent flowing through the VAP and to obtain temperature at a very specific body location. The ECG input may be received from a ECG electrodes mounted on thehousing718/720, thePTC736, and/or theinfusion catheter728. For example,ECG electrodes840 may mounted on abottom surface841 ofbase720 as shown inFIG. 13.

The electronics package and battery source may be hermetically sealed to prevent the electronics from electrically shorting or corroding as a result of water vapor penetration. The battery source762 (rechargeable and/or replaceable) provides the power input (Pwr) to the electronics package. It may comprise a physical battery or a capacitor, for example, and may be implanted with the device or located external to the body and wirelessly coupled to the electronics package by utilizing a magnetic coupling, for example. Such a magnetic coupling may utilize an AC powered primary (external) coil disposed on the skin to create an alternating magnetic field which induces power in a secondary (internal) coil connected to the electronics package and disposed under the skin in close proximity to the primary coil.

Communicating with theprocessor768 viacommunications paths773 is atransmitter774 andreceiver776 pair. In this manner, once a physiological parameter of the body is measured, it can be communicated, in a delayed (requires writable memory connected processor768) or immediate fashion, in a continuous or discrete manner, as processed or raw data, externally to the body so that a practitioner can use the information in treatment of the patient. Preferred transmission methods for the transmitter include, but are not limited to, conduction, radio-frequency waves, magnetic fields, electric fields, sound waves or light waves.

Theprocessor768 may process various information from its inputs, and may be coupled to a memory storage device (not shown). For example, it may derive systolic and diastolic pressures, mean pressures, heart rate and/or respiratory rate in the event its input included blood pressure waveforms from the pressure input. Once processed, the transceiver could send requests to the processor indicative of how often the blood pressure is to be sampled and which parameters are to be extracted, for example. As another example, the processor could evaluate its ECG input for rhythm disturbances.

In a preferred embodiment, thetransceiver770 includes asecond transmitter775 andreceiver777 pair. It is powered by anappropriate power source778 such as an AC or DC source. Viacommunications paths780, thetransmitter775 andreceiver777 communicate with asecond processor782 having amemory784. Theprocessor782 communicates with avisual display786 so that the practitioner can easily see the value of the measured body physiological parameter. In one embodiment, the display can display more than one physiological parameter at a time. In another, it can cycle between pages of displays. Analarm788 is provided to aurally and/or visually indicate that one or more of the measured body physiological parameters has exceeded some acceptably defined range of values. In this manner, the patient and/or practitioner can react swiftly in taking corrective action.

An external connector(s)790 is provided so that the transceiver can become more robust. In various embodiments, the external connector can connect by a direct wire or wireless link, such as by radio-frequency or infrared, to a printer, a general or special purpose computer, additional storage devices, faxes, internet, intranets, cell phone, personal data assistant, satellite, or other such computing or peripheral devices.

It will be appreciated the exact embodiment of thetransceiver770 can embody many forms. For example, in one embodiment it consists of patient strap-on module. In another, it is embodied as a wand to be passed over the patient's skin. In still another, it is coupled physically and electronically together with an infusion pump.

The transmitter and receiver pair of theelectronics package760 and the transmitter and receiver pair of thetransceiver770 may communicate via the use of an antenna associated with thePTC736 orinfusion catheter728. InFIGS. 9A and 9B, and10A and10B, anantenna800 is shown withPTC736. The catheter may have a length (l), and an inner and outer diameter (di and do). Theantenna800 is disposed along a length thereof in a substantially straight manner (as shown), spirally wound manner, or may consist of a plurality of conductors, stranded or braided, to provide flexibility and ruggedness. Aterminal end802 of theantenna800 may be disposed in or adjacent the inner diameter (FIG. 9B), adjacent the-outer diameter. (FIG. 10B), or between the inner and outer diameters (FIG. 10A). In still other embodiments, the antenna is disposed along only a portion of the length of the catheter and a plurality of antennas, instead of just the one shown, are arranged about the inner and outer diameters of the catheter.

The transmitter and receiver pairs may include appropriate modulators, demodulators, amplifiers, oscillators, etc., that are well known and necessary for transmitting and receiving signals, in order to accommodateantenna800. In some embodiments, it will be appreciated that the electronics package only includes a transmitter for communicating externally to the body and does not include a receiver and therefore cannot receive body external information.

With reference toFIGS. 11A-11C, it will be appreciated that the VAP and PMA may, instead of being integrally formed, be combinable with one another before, during or after surgical implantation. In such instances, each of the VAP and the PMA have housings having mating, combinable features. For example, inFIG. 11A, the vascularaccess port housing722 is slidingly engaged with thePMA housing724 viamating slot806 andtab808 features arranged on an

external surface

723,725 of the VAP and PMA, respectively. InFIG. 11B, the two housings are combinable in an interlocking fit configuration as aball810 andsocket812. It will be appreciated that the male/female parts may be switched and are not limited to the embodiments shown. InFIG. 11C, the two housings are combinable as acap814 overbase816 configuration. Still other embodiments include, but are not limited to, one-or-more snap-lock features, tongue-groove configurations, or other known or hereinafter invented arrangements. In still other embodiments, the two housings are compatible shapes but are not positively interlocking, such as with a donut shaped PMA surrounding a donut-hole shaped VAP. It should also be appreciated that in any of the foregoing embodiments, more than one PMA may be combined together with a VAP. Also, when made as combinable housings, flexibility is gained because the VAP and PMA can be made and shipped separate from one another and connected in the operating room upon implantation.

With reference toFIG. 12, another embodiment of a combined VAP and PMA is shown. In this embodiment, thecap718 defines thefluid reservoir754 and themating cap718 andbase720 pair contain both the VAP and the physiological monitoring device. Abezel820 securesinfusion septum734 wheninner ring822 is inserted into thefluid reservoir754. The inner ring is slightly smaller in diameter than the fluid reservoir. Aninner lip824 on theouter ring826 prevents the infusion septum from slipping out of the bezel. Anouter lip828 abuts a top830 of thefluid reservoir754 when the inner ring is inserted therein. An infusionseptum access port742 provides needle access to the infusion septum during use. Aninfusion catheter728 is fluidly interconnected to the fluid reservoir at aproximal end730 for communicating a therapeutic agent from the needle (not shown) to a patient viadistal end732 during use.

Anedge746 of thecap718 mates about awall periphery748 of the base720 to secure the cap and base together. Located between the cap and base, preferably as a hermetically sealed module, is theelectronics package760,battery source762,pressure sensor832 andPTC736. The electronics package and battery source are hemispherically arranged on asubstrate764 to fit within theouter diameter portion834 of thecap718. Suture holes726 are provided to secure the complete apparatus in a patient during use. An antenna, not shown, may also be included with such structure.

InFIG. 13, themating cap718 andbase720 sandwich anelectronics package760,battery source762 on asubstrate764. As input to the physiological monitoring device, a pair ofECG electrodes840 are mounted on abottom surface841 of thebase720. The ECG electrodes monitor an ECG waveform of the patient during use and are implanted in such a manner to achieve this. Electronic interconnections (not shown) provide communications between the electrodes and the electronics package. Thefluid reservoir754 is defined by thecap718 and is fluidly interconnected toinfusion catheter728. APTC736 is coupled to the cap and to the pressure sensor atproximal end738.

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

1. A vascular access port and sensor system, comprising:

a vascular access port including a portal housing; and

a physiological sensor device disposed adjacent the vascular access port, the sensor device including a sensor and a sensor housing, wherein the sensor housing and the portal housing define cooperative geometries.

2. The vascular access port and sensor system ofclaim 1, wherein the vascular access port contains an internal reservoir with first and second openings, a self-sealing septum disposed in the first opening, and a catheter extending from the portal housing, the catheter defining a lumen extending therethrough in fluid communication with the reservoir via the second opening.

3. The vascular access port and sensor system ofclaim 1, wherein the sensor device includes a pressure sensor.

4. The vascular access port and sensor system ofclaim 1, wherein the sensor device includes a temperature sensor.

5. The vascular access port and sensor system ofclaim 1, wherein the sensor device includes an impedance sensor.

6. The vascular access port and sensor system ofclaim 1, wherein the sensor device includes a blood gas sensor.

7. The vascular access port and sensor system ofclaim 1, wherein the sensor device includes an ECG sensor.

8. The vascular access port and sensor system ofclaim 1, wherein the sensor device includes a plurality of sensors.

9. The vascular access port and sensor system ofclaim 1, wherein the sensor housing is fixedly connected to the portal housing.

10. The vascular access port and sensor system ofclaim 9, wherein the sensor housing is integrally formed with the portal housing.

11. The vascular access port and sensor system ofclaim 1, wherein the sensor housing is releasably connected to the portal housing.

12. The vascular access port and sensor system ofclaim 11, wherein the sensor housing interlocks with the portal housing.

13. The vascular access port and sensor system ofclaim 11, wherein the cooperative geometries are defined by a connector extending from the sensor housing and the portal housing.

14. The vascular access port and sensor system ofclaim 13, wherein the connector defines a lumen extending therethrough.

15. The vascular access port and sensor system ofclaim 14, wherein the lumen of the connector is in fluid communication with the internal reservoir.

16. The vascular access port and sensor system ofclaim 1, further comprising a telemetry unit connected to the sensor device.

17. The vascular access port and sensor system ofclaim 16, wherein the sensor generates a sensor signal as a function of a physiological parameter, and wherein the telemetry unit generates a transmission signal as a function of the sensor signal.

18. The vascular access port and sensor system ofclaim 17, further comprising a local data collection system having a communication link with the telemetry unit.

19. The vascular access port and sensor system ofclaim 18, further comprising a remote data collection system having a communication link with the local data collection system.

20. A vascular access port and sensor system, comprising:

a vascular access port including a portal housing containing an internal reservoir with first and second openings, a self-sealing septum disposed in the first opening, a catheter extending from the portal housing, the catheter defining a lumen extending therethrough in fluid communication with the reservoir via the second opening, and a first connector connected to the portal housing; and

a pressure sensor device disposed adjacent the vascular access port, the sensor device including a pressure sensor disposed in a sensor housing, a pressure transmission catheter extending from the sensor housing and being in fluid communication with the pressure sensor, and a second connector connected to the sensor housing;

wherein the first and second connectors define cooperative geometries.

21. The vascular access port and sensor system ofclaim 20, wherein the first and second connectors define mating geometries.

22. The vascular access port and sensor system ofclaim 20, wherein the first and second connectors define interlocking geometries.

23. The vascular access port and sensor system ofclaim 20, wherein the sensor housing and the portal housing are releasably connected.

24. The vascular access port and sensor system ofclaim 20, wherein the sensor housing and the portal housing are fixedly connected.

25. The vascular access port and sensor system ofclaim 20, further comprising a telemetry unit connected to the sensor device.

26. The vascular access port and sensor system ofclaim 25, wherein the pressure sensor generates a sensor signal as a function of blood pressure, and wherein the telemetry unit generates a transmission signal as a function of the sensor signal.

27. A surgical method of implanting a vascular access port and a sensor device, comprising:

providing a vascular access port including a portal housing containing an internal reservoir with first and second openings, a self-sealing septum disposed in the first opening, and a catheter connected to the portal housing, the catheter defining a lumen extending therethrough in fluid communication with the reservoir via the second opening;

providing a physiological sensor device including a sensor and a sensor housing;

surgically forming a subcutaneous pocket through an incision;

introducing the catheter of the vascular access port into a vascular lumen;

placing the portal housing is the subcutaneous pocket;

placing the sensor device in the subcutaneous pocket; and

surgically closing the incision.

28. The surgical method ofclaim 27, wherein the sensor device is placed adjacent the vascular access port.

29. The surgical method ofclaim 27, wherein the sensor housing and the portal housing define cooperative geometries, and wherein the cooperative geometries are placed immediately adjacent each other.

30. The surgical method ofclaim 27, wherein the sensor housing and the portal housing define interlocking geometries, and wherein the interlocking geometries are interlocked with each other.

31. The surgical method ofclaim 27, wherein the sensor housing and the portal housing are releasably connected to each other.

32. The surgical method ofclaim 27, wherein the sensor housing and the portal housing are fixedly connected to each other.

33. The surgical method ofclaim 27, further comprising:

providing a telemetry unit connected to the sensor device; and

placing the telemetry unit in the subcutaneous pocket.

34. A medical treatment method, comprising:

implanting the vascular access port and the sensor device;

administering a therapeutic agent through the vascular access port; and

monitoring a physiological measure using the sensor device.

35. The medical treatment method ofclaim 34, further comprising:

changing the administration of the therapeutic agent as a function of the monitored physiological measure.

36. The medical treatment method ofclaim 34, further comprising:

providing a telemetry unit connected to the sensor device;

implanting the telemetry unit;

wherein the sensor device generates a sensor signal as a function the physiological measure; and

wherein the telemetry unit generates a transmission signal as a function the sensor signal.

37. A sensor device for use with a vascular access port including a portal housing having a geometry, the sensor device comprising:

a sensor housing;

a physiological sensor disposed in the sensor housing;

wherein the sensor housing defines a geometry that is cooperative with the geometry of the portal housing.

38. The sensor device ofclaim 37, further comprising a telemetry unit carried by the sensor housing.

39. A vascular access port for use with a sensor device including a sensor housing having a geometry, the vascular access port comprising:

a portal housing containing an internal reservoir with first and second openings;

a self-sealing septum disposed in the first opening; and

a catheter extending from the portal housing, the catheter defining a lumen extending therethrough in fluid communication with the reservoir via the second opening;

wherein the portal housing defines a geometry that is cooperative with the sensor housing.