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US3639084A - Mechanism for control pulsatile fluid flow - Google Patents

Mechanism for control pulsatile fluid flowDownload PDF

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US3639084A
US3639084AUS25782AUS3639084DAUS3639084AUS 3639084 AUS3639084 AUS 3639084AUS 25782 AUS25782 AUS 25782AUS 3639084D AUS3639084D AUS 3639084DAUS 3639084 AUS3639084 AUS 3639084A
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fluid
space
pressure
conduit
pulsatile
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US25782A
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Richard Paul Goldhaber
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Baxter International Inc
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Baxter Laboratories Inc
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Abstract

This application relates to an apparatus for imparting a pulsatile flow to fluid in a conduit, which has pumping means for providing the pulsatile flow of fluid therein. The apparatus includes an elastic tubular section defining a portion of the conduit and located downstream of the pulsatile flow providing means. The tubular section is surrounded by a sealed sleeve to define a pressurizable space about the tubular section. The space is pressurizable so that the pulsatile flow pattern of fluid passing through the tubular section is controlled in a manner responsive to the pressure within said space. If desired, a portion of the flow conduit upstream of the pumping means is of enlarged transverse dimension and sealed within a second sleeve to define a second pressurizable space to provide a means for increasing the flow of fluid into the pulsatile pumping means.

Description

United States Patent 1 1 3,639,084
Goldhaber 1 Feb. 1, 1972 [54] MECHANISM FOR CONTROL OTHER PUBLICATIONS PULSATILE FLUID FLOW [72] Inventor: Richard Paul Goldhaber, Chicago, Ill.
[73) Assignee: Baxter Laboratories, Inc., Morton Groove,
Ill.
[22] Filed: Apr. 6, 1970 [211 App]. No; 25,782
l52| US. Cl ..4l7/394, l28/l,23/258.5, l95/l .7 [511 Int. Cl. ..F04b 43/10,F04b 45/00, Afilb lQ/OO, A6lm [58] Field ol'Search l28/l DIG. 3; 23/2585; I95/l.7; 417/395, 394, 540. 53, 542
[56] References Cited UNITED STATES PATENTS 2,405,734 8/1946 Coe ..4l7/395 3.490.438 l/l970 Lavender et al. ..l28/l R The Lancet-Jan. 25, I958, page I97 By Rotellar Primary Examiner-Robert M. Walker Attorney-Walter C. Kehm and W. Garrettson Ellis ABSTRACT This application relates to an apparatus for imparting a pulsatilc flow to fluid in a conduit, which has pumping means for providing the pulsatile flow of fluid therein The apparatus includes an elastic tubular section defining a portion of the conduit and located downstream of the pulsatile flow providing means The tubular section is surrounded by a sealed sleeve to define a pressurizable space about the tubular section. The space is pressurizable so that the pulsatile flow pattern of fluid passing through the tubular section is controlled in a manner responsive to the pressure within said space. If desired, a portion of the flow conduit upstream of the pumping means is of enlarged transverse dimension and sealed within a second sleeve to define a second pressurizable space to provide a means for increasing the flow of fluid into the pulsatile pumping means.
6 Claims, 3 Drawing Figures Pmmmm um 3539.084
SHEEI 1 BF 2 [220622 far MECHANISM FOR CONTROL PULSATILE FLUID FLOW BACKGROUND OF THE INVENTION Equipment for providing a pulsatile flow of fluid through a conduit is currently used in experimental and clinical work relating to organ perfusion and the like. it has been found that the life span of surgically removed living organs, such as livers, hearts, or kidneys, can be prolonged by perfusing the organs with an oxygenated solution. In particular, it has been found that the viability of such separated organs is prolonged by perfusing them with oxygenated solution in a pulsatile flow pattern simulating the beating of the heart.
While several systems for providing a pulsatile flow of oxygenated fluid to living organs have been constructed, deficiencies have been noted in that the prior art devices are unable to provide a wide variation of pulsatile flow patterns, so that the user can select the precise amplitude and shape of the pulsatile flow pressure waves desired. Also, the pumps which provide pulsatile flow do not operate with an optimum volume of flow.
DESCRIPTION OF THE INVENTION The invention of this application provides a simple means for controlling the pattern of pulsatile flow of fluid through a conduit, permitting the alteration of both the amplitude and shape of the pulse or pressure wave as measured against time. Furthermore, this application provides a means for providing increased volumes of fluid through a narrow conduit to the pulsatile flow pump for greater pumping efficiencies.
In accordance with this invention, an apparatus for imparting flow to fluid in a conduit is provided, having pump means for providing a pulsatile pressure to cause flow of fluid in said conduit. The apparatus contains aorta means comprising an elastic tubular section defining a portion of the conduit. The tubular section is located downstream of the pulsatile flow providing means, and is surrounded by a sealed sleeve to define a pressurizablc space about the section. The space within the sleeve is pressurizable as desired to alter the compliance of the tubular section by controllable pressure to any degree and in any pattern desired. Hence, the pulsatile flow pattern of fluid passing through the sleeve having pulsations provided by the pulsatile pump means is modulated in a manner responsive to the pressure within the space about the sleeve. For example. a constant pressure can be used, or an in phase oscillatory pressure to augment the amplitude and alter the shape of the pulsations, or an out-of-phase oscillatory pressure to reduce, modify, or even eliminate, the pulsations. As a result of this, the ultimate flow pattern is controllable by the selective controlling of the pressure within the space about the tubular section as described further below.
The tubular sections used herein can be of any cross section defining a closed figure, e.g., round, oval, or the like.
Furthermore, a portion of the fluid flow conduit located directly upstream of and communicating with the inlet of the pulsatile pump means can define an atrium space of enlarged transverse dimension to provide a greater pulsatile flow efficiency, in accordance with the teachings of Anderson, et al., American Heart Journal, Jan, I967, pages 92-105.
In accordance with this invention, the portion ofthe conduit defining the atrium space is surrounded by a second sealed sleeve to define a second pressurizable space about the portion of conduit. The second space is pressurized with oscillatory pressure which causes the atrium space to collapse during the filling phase of the pulsatile pumping means and to expand during the pumping phase of the pulsatile pumping means. Thus, abundant fluid is provided to the pulsatile pumping means, resulting in greater pumping efficiency.
Referring to the drawings:
FIG. I is a schematic view of an organ preservation system in accordance with this invention.
FIG. 2 is a view, taken in vertical section, of the pulsatile pumping means and related portions used in this invention.
FIG. 3 is a partial vertical sectional view of another embodi ment ofthe atrium space and the pulsatile pumping means.
Referring to the drawings, an organ perfusion system is shown in which perfusate fluid, for example blood or plasma, is pumped through a typically transparentorgan preservation chamber 10 to permit viewing of the organ. The fluid is driven by a pulsatile pump [2 throughconduit 14 intochamber 10, through a cannulated organ contained therein, and then outconduit 16. Accessport 17 is provided in organ chamber [0 for use as needed.Port 17 can be connected to the organ to conduct organ secretions out of the chamber [0 to an accumulating container (not shown if desired. The perfusate flow path of the organ preservation system is disposed in a hyperbaric chamber, if desired, for hyperbaric perfusion. The device can include a compact container for easy transportability.
The liquid perfusate is conducted uniformly from the organ in chamber [0 through conduit [6 to aconventional heat exchanger 18, in which the temperature of the pcrfusate is brought to a desired temperature, generally between 4 and about 37 C. to control the temperature within the system. A separate circuit forheat exchanger fluid 20 passes into close heat exchanging relation with the perfusate passing into the heat exchanger from conduit l6, but the two fluids are separated by a thin metal heat transfer partition. Heat exchange fluid such as saline is circulated inconduits 22 betweenheat exchanger 18 and a conventional temperature control source andpump 24.
Perfusate at a desired temperature passes fromheat exchanger 18 viaconduit 26 to a conventional oxygenator 28 (such as described in Belgian Pat. No. 726,886) for transferring oxygen to and expelling carbon dioxide from the perfusate.Oxygenator 28 also contains an oxygen flow pathcom prising line 30 andexhaust line 32. From the oxygenator the perfusate is passed throughconduit 34 and sealedconnection 36 into an enlarged portion of the conduit which definesatri um space 38, typically made of flexible, limp, thin-walled rubber tubing.Atrium space 38 provides a flexible storage chamber for perfusate to accumulate between filling phases of thepulsatile pump 12, and is surrounded bytubular guard 37.
The amount of perfusate flowing in the system is regulated by adding perfusate as needed from reservoir 4!, controlled byvalve 43, to compensate for liquid lost as secretions throughport 17 and the like.
As shown in H0. 2,pulsatile pump 12 comprises acylinder 42 containing anelastic tube 44 positioned axially withincylinder 42. Thespace 45 betweentube 44 andcylinder 42 is sealed byannular seals 47, 49 to define a sealed annular chamber. lnlet means 46 and outlet means 48 from the pump each include a one-way leaf-type flap valve 50, each of which opens to permit flow intotube 44 throughinlet 46 and outoutlet 48 while preventing backflow of fluid.
Cylinder 42 defines anentrance port 52 to receive fluid from an oscillatory pressure providing system, which includestube 54 containing a head ofhydraulic fluid 56 and which is connected throughline 58 to a conventional oscillatory pressure generating control source 60 (FIG. I), operated bygas supply 61, typically oxygen.Control source 60 is shown to provide oscillatory oxygen pressure toline 58, and also to provide an oxygen flow tooxygenator 28, typically using oxygen passing through a flowmeter incontrol source 60. The oscillatory pressure causes fluid to pass back and forth throughport 52 to aspace 45 withincylinder 42 and outside oftube 44 to actuatepump 12 by alternately collapsingtube 44 and permitting it to expand again in accordance with the pressure and relaxation cycles of the oscillatory pressure. Astube 44 collapses, fluid is forced out of outlet means 48 in each pumping phase, and astube 44 expands, fluid passes in through inlet means 46 in each filling phase. Typically,pump 12 is positioned at a vertically lower position than organ chamber [0 to provide a hydrostatic pressure head of fluid to assist in filling oftube 44 during the filling phase.Oxygenator 28 is also positioned vertically lower than chamber [0 for pressurization there.
A suitablepneumatic control source 60 for providing oscillatory pressure toline 58 andentrance port 52 is disclosed in the article by Demers et al., entitled A Perfusion Circuit for Organ Preservation in Portable Chambers." J. Surgical Research, vol. 9, No. 2, pp. 95-99 (1969). This article also refers to a suitable combined heat exchangeroxygenator which can be used in substitution for the separate members [8 and 28 in this invention. This or other pneumatic systems can be adjusted to provide the desired period between pulses.
In accordance with this invention, anelastic tubular section 62 defines a portion of the conduit for pulsatile flow of fluid, and is located downstream ofpulsatile pump 12. Tubular sec'tion 62 is surrounded by a sealedsleeve 64, integral withcylinder 42, to define apressurizable space 66 betweensleeve 64 andtubular section 62.Line 68 leads betweenspace 66 and a pressure control 70 (FIG. I] which connects to pressurized oxygen source 6| vialine 72.
Pressure control 70 can be a simple constant pressure regulator, or, if desired, can be a source of variable pressure, coor' dinated, if desired, with the oscillatory pressure provided bysource 60. As fluid is forced out ofpump 12 in a pulse of pressure, the amplitude and shape of the pressure wave can be varied by varying the resilience or compliance oftubular sec tion 62. This resilience, or compliance, is controlled as desired by controlling the pressure provided throughline 68, thus varying the capacity oftubular section 62 to receive perfusate. If high pressure is provided, the compliance characteristics oftube 62, when exposed to the pressure wave passing out of pump [2, are quite different from the compliance charac teristics oftube 62 when there is a low pressure or a reduced pressure withinconduit 68 andspace 66. A constant pressure can be provided withinspace 66, as well as an oscillatory pres sure of any type desired, either in phase or out of phase with the oscillatory pressure used to drive pump I2. Thus great flexibility is available in the control of the shape of the pressure pulse of the oscillatory fluid flow passing throughconduit 14 to organ chamber I0.
Referring to FIG. 3, there is shown a modification of a device which is otherwise similar to the device of FIGS. I and 2 except as stated. The portion of conduit definingatrium space 38 and disposed within guard orsleeve 37 is sealed bycap 70 to define anotherpressurizable space 72. The conduit definingatrium chamber 38 is typically glued to cap 70 at 74 to make the space fluidtight.Line 76 leads betweenspace 72 and a source of oscillatory pressure such assource 60. The pressure oscillations inspaces 45 and 72 are arranged to be out of phase with each other, generally with the pulses inspace 72 shortly preceding the pulses inspace 45. Hence, aselastic tube 44 of pump I2 is in the filling phase of its pumping cycle for receiving fluid throughinlet 46,line 76 is providing a pulse of pressure tospace 72 to collapse the conduit definingatrium space 38 to force fluid into pump I2. No check valve is needed to prevent excessive backflow of fluid fromatrium space 38. The majority of fluid inatrium space 38 passes into pump I2 without such a valve becauseinlet 46 is wider thanconduit 34 and because the pressure inconduit 34 caused by the elevated organ chamber is greater than the pressure withintube 44 during the filling cycle, because ofthe inherent resiliency of the tube and its tendency to spring back to its uncollapsed position, For greater efficiency, a check valve can be provided, ifdesired.
Out of phase oscillatory pressure is provided tospace 45 throughline 78 andport 79 by a conventional time delay device connected to line 76 to operate a pilot valve inline 78 which opens the line in one position and closes, but permits backward venting, in another position, to provide oscillatory pressure intube 80 andspace 45.Line 78 is then connected to a pressure source such asoxygen supply 61, to provide a constant pressure to line 78 upstream ofthe pilot valve A typical time delay device can constitute a conduit c0n nectcd toline 76, running through a chamber of predetermined volume, and then past an adjustable needle valve to a pressure responsive switching control of the pilot valve. The
size of the chamber and the needle valve are adjusted to give I the desired time delay A suitable pilot valve is available from the Fluidonics Division of Imperial Eastman Corporation of Chicago, Illinois under the part number 3001 35.
During the pumping phase of pump I2 in FIG. 3,flap valve 50 ofinlet 46 is closed, and the oscillatory pressure inspace 72 andline 76 is at a reduced level to permit the conduit which definesatrium chamber 38 to fill once again with perfusate.
The pressure pattern inspace 72 can be arranged so that the duration of each pressure pulse with collapses the portion of conduit definingatrium space 38 lasts for only a portion of thefilling phase oftube 44.
In a specific embodiment, the oscillatory pressure inline 76 has a maximum pressure of about 20 mm. Hg, while the oscillatory pressure provided tolines 58 or 78 and from thence to pump [2 has a maximum pressure of about IOU mm. Hg. The frequency of oscillation for both oscillatory pressures is, for example, 60 cycles per minute. The pressure provided inline 68 can be constant at 20 mm, Hg. A constant pressure of this level inline 68 assures that a minimum bias diastolic pressure is constantly present in the system between pulsations of flow, and particularly that such minimum bias pressure is imposed upon the organ within chamber I0 through line l4. It is believed that this prolongs organ viability.
The parts which contact the perfusate are typically made of silicone rubber to be atraumatic to blood.
The apparatus of this invention can use any fluid inconduit 68 and the space betweentubular section 62 andsleeve 64, and in the other pressurizable areas, depending upon the com pliance characteristics desired. Liquids of varying viscosity such as oil, silicone fluid, or water, provide differing compliance characteristics, which in turn differ from the compliance characteristics of gases. An incompressible liquid such as saline can be used, while closing offconduit 68, to provide very little compliance totubular section 62, in which there is very little damping or modulation of the pressure pulses passing therethrough.
The above specific disclosure is for illustrative purposes only and is not for purposes of limiting the scope of the invention of this application. Broadly, the invention of this applica tion can be utilized in many different devices, including organ perfusion apparatus comprising (a) container means for receiving an organ; (b) means for delivering perfusate to the organ within the container, (c) means for developing pulsatile pressure in the perfusate delivered to the organ; (0') means for imposing a minimum pressure bias on perfusate circulated through the organ between pressure pulses; (e) means for oxygenating perfusate conducted from the organ; and (1') control means for determining the pump output, the control means comprising means for setting the period of each high pressure pulse.
Manual control means can be provided to vary the temperatu re and pressure of perfusate provided to the organ, as well as for regulating the pulse rate and systole period of each pulse developed by the pump means.
That which is claimed is:
l In an organ perfusion apparatus for passing fluid in a conduit through an organ in a container including pump means for providing a pulsatile pressure to cause flow of fluid in said conduit, in which said pump means comprises a cylinder con taining an elastic tube positioned axially therein, means for sealing the interior of said tube from the exterior thereof to define a sealed flow path for fluid to be pumped, and inlet and outlet means to allow said fluid to pass through the tube, said inlet and outlet means each containing a one-way valve to prevent backflow of fluid, said cylinder defining an entrance port to receive fluid within the cylinder and outside said tube from first oscillatory pressure providing means, to actuate said pulsatile pressure providing means by repeatedly collapsing said tube and permitting it to expand again by application of oscillatory pressure, in which a portion of said conduit defines an atrium space of enlarged transverse dimension, said atrium space being located directly upstream of and extending to said inlet means of the pump means, in which said atrium space is surrounded by a second sealed sleeve to define a second pres surizable space about said portion of conduit, and in which said second sleeve has second means for pressurizing said second space with oscillatory pressure which is out of phase from the oscillatory pressure provided by said first oscillatory pressure providing means, so that when the elastic tube of the pump means is in its filling phase. the portion of conduit defining said atrium space is in its collapsing phase to provide pressurized fluid to said inlet means. for greater pumping efficien- 2. The organ perfusion apparatus of claim 1 in which an elastic tubular section defines a portion of said conduit and is located between said pump means and said organ container. the elastic tubular section being surrounded by a sealed sleeve to define a pressurizable space about said tubular section, and
means for controlling the pressure in said space. whereby the pulsatile flow pattern of fluid passing through said tubular section is controlled in a manner responsive to the pressure within said space.
3. The apparatus of claim 2 in which said elastic tubular section is positioned downstream of and adjacent to said pulsatile pressure providing means.
4. The apparatus of claim 2 in which said conduit for pulsatile fluid flow defines a closed loop circuit.
5. The apparatus of claim 2 in which said sealed sleeve and said cylinder define a single. integral member.
6. An organ perfusion device incorporating the apparatus defined in claim 2.

Claims (6)

1. In an organ perfusion apparatus for passing fluid in a conduit through an organ in a container including pump means for providing a pulsatile pressure to cause flow of fluid in said conduit, in which said pump means comprises a cylinder containing an elastic tube positioned axially therein, means for sealing the interior of said tube from the exterior thereof to define a sealed flow path for fluid to be pumped, and inlet and outlet means to allow said fluid to pass through the tube, said inlet and outlet means each containing a one-way valve to prevent backflow of fluid, said cylinder defining an entrance port to receive fluid within the cylinder and outside said tube from first oscillatory pressure providing means, to actuate said pulsatile pressure providing means by repeatedly collapsing said tube and permitting it to expand again by application of oscillatory pressure, in which a portion of said conduit defines an atrium space of enlarged transverse dimension, said atrium space being located directly upstream of and extending to said inlet means of the pump means, in which said atrium space is surrounded by a second sealed sleeve to define a second pressurizable space about said portion of conduit, and in which said second sleeve has second means for pressurizing said second space with oscillatory pressure which is out of phase from the oscillatory pressure provided by said first oscillatory pressure providing means, so that when the elastic tube of the pump means is in its filling phase, the portion of conduit defining said atrium space is in its collapsing phase to provide pressurized fluid to said inlet means, for greater pumping efficiency.
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Cited By (62)

* Cited by examiner, † Cited by third party
Publication numberPriority datePublication dateAssigneeTitle
US3877843A (en)*1973-05-211975-04-15Baxter Laboratories IncPulsatile pumping system
US4080958A (en)*1976-02-271978-03-28Datascope CorporationApparatus for aiding and improving the blood flow in patients
US4250872A (en)*1978-05-251981-02-17Yehuda TamariBlood pulsating and/or pumping device
US4395492A (en)*1981-06-031983-07-26Res-Del Group Ltd.Perfusion chamber
US4417861A (en)*1981-08-101983-11-29Monsanto CompanyCell culture pumping system
US4573883A (en)*1985-03-011986-03-04Baylor College Of MedicineDisposable blood pump
US4769241A (en)*1986-09-231988-09-06Alpha Therapeutic CorporationApparatus and process for oxygenation of liquid state dissolved oxygen-carrying formulation
US4782817A (en)*1987-05-291988-11-08Abiomed Cardiovascular, Inc.Ventricular support system
US5141847A (en)*1989-08-181992-08-25Kureha Chemical Industry Co., Ltd.Method and apparatus for producing pulsation
US5338662A (en)*1992-09-211994-08-16Bio-Preserve Medical CorporationOrgan perfusion device
US5472876A (en)*1991-07-081995-12-05The American National Red CrossComputer controlled cryoprotectant perfusion apparatus
US5537335A (en)*1993-11-011996-07-16University Of Pittsburgh Of The Commonwealth System Of Higher EducationFluid delivery apparatus and associated method
WO1997045527A1 (en)*1996-05-291997-12-04Trans D.A.T.A. Service, Inc.Portable perfusion/oxygenation module having respiratory gas driven, mechanically linked dual pumps and mechanically actuated flow control valve for slow pulsatile cycling of oxygenated perfusate during in vitro conservation of viable transplant organs
US5723282A (en)*1991-07-081998-03-03The American National Red CrossMethod of preparing organs for vitrification
US5856081A (en)*1991-07-081999-01-05The American National Red CrossComputer controlled cryoprotectant perfusion apparatus
US5916800A (en)*1995-06-071999-06-29St. June Medical, Inc.Cardiovascular bioreactor apparatus and method
US6342214B1 (en)*1995-05-162002-01-29Karl TryggvasonMethod for viral vector delivery
US6345962B1 (en)*2000-05-222002-02-12Douglas E. SutterFluid operated pump
WO2002089571A1 (en)*2001-05-042002-11-14Breonics, Inc.Organ chamber for exsanguinous metabolic support system
US6582953B2 (en)*1999-04-142003-06-24Breonics, Inc.Organ chamber for exsanguinous metabolic support system
US6638264B1 (en)1995-05-162003-10-28Biostratum IncorporationPerfusion apparatus and methods for pharmaceutical delivery
US6642045B1 (en)*1997-04-142003-11-04Breonics, Inc.System for exsanguinous metabolic support of an organ or tissue
US6673594B1 (en)1998-09-292004-01-06Organ Recovery SystemsApparatus and method for maintaining and/or restoring viability of organs
US20040221719A1 (en)*2003-04-042004-11-11Organ Recovery Systems, Inc.Device for separating gas from a liquid path
US20040224299A1 (en)*2003-04-042004-11-11Organ Recovery SystemsMethod and apparatus for transferring heat to or from an organ or tissue container
US20040224298A1 (en)*1998-09-292004-11-11John BrassilApparatus and method for determining effects of a substance of an organ
US20040241634A1 (en)*2003-06-022004-12-02Organ Recovery SystemsMethod and apparatus for pressure control for maintaining viability of organs
US20050147958A1 (en)*1997-09-232005-07-07Waleed HassaneinCompositions, method and devices for maintaining an organ
US20050221269A1 (en)*2004-04-052005-10-06Organ Recovery SystemsApparatus and method for perfusing an organ or tissue for isolating cells from the organ or tissue
US20060063142A1 (en)*1998-09-292006-03-23Organ Recovery Systems, Inc.Apparatus and method for maintaining and/or restoring viability of organs
US20060148062A1 (en)*2004-10-072006-07-06Transmedics, Inc.Systems and methods for ex-vivo organ care
US20060154357A1 (en)*2004-10-072006-07-13Transmedics, Inc.Systems and methods for ex-vivo organ care
US7326564B2 (en)2001-02-202008-02-05St. Jude Medical, Inc.Flow system for medical device evaluation and production
US20080234768A1 (en)*2007-03-202008-09-25Transmedics, IncSystems for monitoring and applying electrical currents in an organ perfusion system
WO2009020412A1 (en)*2007-07-062009-02-12Xenodevice AbSystem and method for organ evaluation and preservation
US20090197240A1 (en)*2008-01-312009-08-06Transmedics, IncSystems and methods for ex vivo lung care
US20090202977A1 (en)*2005-08-262009-08-13Regents Of The University Of MinnesotaDecellularization and recellularization of organs and tissues
WO2010014928A2 (en)2008-08-012010-02-04Biomedinnovations, LlcMethods and apparatus for organ support
US20100093066A1 (en)*2005-08-262010-04-15Regents Of The University Of MinnesotaDecellularization and recellularization apparatuses and systems containing the same
US20100316705A1 (en)*1999-04-142010-12-16Lauren BrasileSystem for exsanguinous metabolic support of an organ or tissue
US20110104651A1 (en)*2009-11-042011-05-05Sweeney Terrence EMechanical Model of the Cardiovascular System and Method of Demonstrating the Physiology of the Cardiovascular System
US20110136096A1 (en)*2006-04-192011-06-09Transmedics, Inc.Systems and Methods for Ex Vivo Organ Care
US20130004369A1 (en)*2010-01-132013-01-03Oliver MarseilleArrangement with a blood pump and a gas exchanger for extracorporeal membrane oxygenation
US20130217128A1 (en)*2005-02-172013-08-22Technische Universiteit EindhovenMethod of manufacturing a tissue-engineered prosthesis
US20140135697A1 (en)*2011-06-202014-05-15Veinux ApsDisposable heat exchange cassette and an assembly for heating intravenous fluid
US9078428B2 (en)2005-06-282015-07-14Transmedics, Inc.Systems, methods, compositions and solutions for perfusing an organ
US9290738B2 (en)2012-06-132016-03-22Miromatrix Medical Inc.Methods of decellularizing bone
US9881523B2 (en)2009-11-042018-01-30University Of ScrantonMechanical model of the cardiovascular system and method of demonstrating the physiology of the cardiovascular system
US9894894B2 (en)2004-10-072018-02-20Transmedics, Inc.Systems and methods for ex-vivo organ care and for using lactate as an indication of donor organ status
US10076112B2 (en)2014-06-022018-09-18Transmedic, Inc.Ex vivo organ care system
US10194655B2 (en)2015-09-092019-02-05Transmedics, Inc.Aortic cannula for ex vivo organ care system
US10233420B2 (en)2010-09-012019-03-19Regents Of The University Of MinnesotaMethods of recellularizing a tissue or organ for improved transplantability
US11278643B2 (en)2016-09-062022-03-22Mayo Foundation For Medical Education And ResearchUse of resected liver serum for whole liver-engineering
US11452797B2 (en)2013-03-152022-09-27Miromatrix Medical Inc.Use of perfusion decellularized liver for islet cell recellularization
US11856944B2 (en)2011-04-142024-01-02Transmedics, Inc.Organ care solution for ex-vivo machine perfusion of donor lungs
US11963526B2 (en)2014-12-122024-04-23Transmedics, Inc.Apparatus and method for organ perfusion
US11998662B1 (en)2021-06-092024-06-04Reprise Biomedical, Inc.Biologic matrix for a wound site and related methods
US12010987B2 (en)2004-10-072024-06-18Transmedics, Inc.Systems and methods for ex-vivo organ care and for using lactate as an indication of donor organ status
US12127554B2 (en)2016-05-302024-10-29Transmedics, Inc.Apparatus and method for ex vivo lung ventilation with a varying exterior pressure
US12263275B2 (en)2018-06-132025-04-01Miromatrix Medical Inc.Fistula filler and deployment system
US12280192B2 (en)2017-09-202025-04-22Hemovent GmbhGas exchange unit
US12383657B1 (en)2021-06-092025-08-12Reprise Biomedical, Inc.Biologic matrix for a wound site and related methods

Families Citing this family (1)

* Cited by examiner, † Cited by third party
Publication numberPriority datePublication dateAssigneeTitle
GB2327715B (en)*1997-07-242001-11-21Peter John KimberPumping of fluids

Citations (2)

* Cited by examiner, † Cited by third party
Publication numberPriority datePublication dateAssigneeTitle
US2405734A (en)*1944-08-191946-08-13Harrison S CoePumping apparatus
US3490438A (en)*1967-06-081970-01-20Atomic Energy CommissionPerfusion chamber and cannulae therefor

Patent Citations (2)

* Cited by examiner, † Cited by third party
Publication numberPriority datePublication dateAssigneeTitle
US2405734A (en)*1944-08-191946-08-13Harrison S CoePumping apparatus
US3490438A (en)*1967-06-081970-01-20Atomic Energy CommissionPerfusion chamber and cannulae therefor

Non-Patent Citations (1)

* Cited by examiner, † Cited by third party
Title
The Lancet Jan. 25, 1958, page 197 By Rotellar*

Cited By (154)

* Cited by examiner, † Cited by third party
Publication numberPriority datePublication dateAssigneeTitle
US3877843A (en)*1973-05-211975-04-15Baxter Laboratories IncPulsatile pumping system
US4080958A (en)*1976-02-271978-03-28Datascope CorporationApparatus for aiding and improving the blood flow in patients
US4250872A (en)*1978-05-251981-02-17Yehuda TamariBlood pulsating and/or pumping device
US4395492A (en)*1981-06-031983-07-26Res-Del Group Ltd.Perfusion chamber
US4417861A (en)*1981-08-101983-11-29Monsanto CompanyCell culture pumping system
US4573883A (en)*1985-03-011986-03-04Baylor College Of MedicineDisposable blood pump
US4919895A (en)*1986-09-231990-04-24Alpha Therapeutic CorporationApparatus for oxygenation of liquid state dissolved oxygen-carrying formulation
US4769241A (en)*1986-09-231988-09-06Alpha Therapeutic CorporationApparatus and process for oxygenation of liquid state dissolved oxygen-carrying formulation
US4782817A (en)*1987-05-291988-11-08Abiomed Cardiovascular, Inc.Ventricular support system
US5141847A (en)*1989-08-181992-08-25Kureha Chemical Industry Co., Ltd.Method and apparatus for producing pulsation
US5821045A (en)*1991-07-081998-10-13The American National Red CrossMethods for removal of cryoprotectant from organs prior to transplantation
US5472876A (en)*1991-07-081995-12-05The American National Red CrossComputer controlled cryoprotectant perfusion apparatus
US6187529B1 (en)1991-07-082001-02-13The American National Red CrossMethod for preparing organs for transplantation after cryopreservation
US5962214A (en)*1991-07-081999-10-05The United States Of America As Represented By The American National Red CrossMethod of preparing tissues and cells for vitrification
US5856081A (en)*1991-07-081999-01-05The American National Red CrossComputer controlled cryoprotectant perfusion apparatus
US5723282A (en)*1991-07-081998-03-03The American National Red CrossMethod of preparing organs for vitrification
US5494822A (en)*1992-09-211996-02-27Bio-Preserve Medical CorporationOrgan perfusion device
US5338662A (en)*1992-09-211994-08-16Bio-Preserve Medical CorporationOrgan perfusion device
US5537335A (en)*1993-11-011996-07-16University Of Pittsburgh Of The Commonwealth System Of Higher EducationFluid delivery apparatus and associated method
US6638264B1 (en)1995-05-162003-10-28Biostratum IncorporationPerfusion apparatus and methods for pharmaceutical delivery
US6342214B1 (en)*1995-05-162002-01-29Karl TryggvasonMethod for viral vector delivery
US5916800A (en)*1995-06-071999-06-29St. June Medical, Inc.Cardiovascular bioreactor apparatus and method
US6174719B1 (en)1995-06-072001-01-16St. Jude Medical, Inc.Cardiovascular bioreactor apparatus and method
WO1997045527A1 (en)*1996-05-291997-12-04Trans D.A.T.A. Service, Inc.Portable perfusion/oxygenation module having respiratory gas driven, mechanically linked dual pumps and mechanically actuated flow control valve for slow pulsatile cycling of oxygenated perfusate during in vitro conservation of viable transplant organs
US5965433A (en)*1996-05-291999-10-12Trans D.A.T.A. Service, Inc.Portable perfusion/oxygenation module having mechanically linked dual pumps and mechanically actuated flow control for pulsatile cycling of oxygenated perfusate
US6642045B1 (en)*1997-04-142003-11-04Breonics, Inc.System for exsanguinous metabolic support of an organ or tissue
US9756851B2 (en)1997-09-232017-09-12The Department Of Veteran AffairsCompositions, methods and devices for maintaining an organ
US20050147958A1 (en)*1997-09-232005-07-07Waleed HassaneinCompositions, method and devices for maintaining an organ
US8409846B2 (en)*1997-09-232013-04-02The United States Of America As Represented By The Department Of Veteran AffairsCompositions, methods and devices for maintaining an organ
US9756850B2 (en)1997-09-232017-09-12The Department Of Veteran AffairsCompositions, methods and devices for maintaining an organ
US9756849B2 (en)1997-09-232017-09-12The Department Of Veteran AffairsCompositions, methods and devices for maintaining an organ
US20110053256A1 (en)*1998-09-292011-03-03Lifeline Scientific, Inc.Apparatus and method for maintaining and/or restoring viability of organs
US8420381B2 (en)1998-09-292013-04-16Lifeline Scientific, Inc.Apparatus and method for maintaining and/or restoring viability of organs
US7749693B2 (en)1998-09-292010-07-06Lifeline Scientific, Inc.Method of determining that an organ is not suitable for transplantation and using it for testing substances
US20110039253A1 (en)*1998-09-292011-02-17Lifeline Scientific, Inc.Apparatus and method for maintaining and/or restoring viability of organs
US8268547B2 (en)1998-09-292012-09-18Lifeline Scientific, Inc.Method of transporting and storing a kidney
US20110059429A1 (en)*1998-09-292011-03-10Lifeline Scientific, Inc.Apparatus and method for maintaining and/or restoring viability of organs
US20100221696A1 (en)*1998-09-292010-09-02Organ Recovery Systems, Inc.Apparatus and method for maintaining and/or restoring viability of organs
US20060063142A1 (en)*1998-09-292006-03-23Organ Recovery Systems, Inc.Apparatus and method for maintaining and/or restoring viability of organs
US8268612B2 (en)1998-09-292012-09-18Lifeline Scientific, Inc.Apparatus and method for maintaining and/or restoring viability of organs
US8318415B2 (en)1998-09-292012-11-27Lifeline Scientific, Inc.Method of determining transport and/or storage parameters for maintaining viability of an organ
US8349551B2 (en)1998-09-292013-01-08Lifeline Scientific, Inc.Method for controlling perfusion of an organ
US6673594B1 (en)1998-09-292004-01-06Organ Recovery SystemsApparatus and method for maintaining and/or restoring viability of organs
US8962303B2 (en)1998-09-292015-02-24Lifeline Scientific, Inc.Apparatus and method for maintaining and/or restoring viability of organs
US8609400B2 (en)1998-09-292013-12-17Lifeline Scientific, Inc.Apparatus and method for maintaining and/or restoring viability of organs
US8445260B2 (en)1998-09-292013-05-21Lifeline Scientific, Inc.Apparatus and method for maintaining and/or restoring viability of organs
US8431385B2 (en)1998-09-292013-04-30Lifeline Scientific, Inc.Apparatus and method for maintaining and/or restoring viability of organs
US20040224298A1 (en)*1998-09-292004-11-11John BrassilApparatus and method for determining effects of a substance of an organ
US20110129908A1 (en)*1998-09-292011-06-02Lifeline Scientific, Inc.Apparatus and method for maintaining and/or restoring viability of organs
US7824848B2 (en)1998-09-292010-11-02Lifeline Scientific, Inc.Apparatus and method for maintaining and/or restoring viability of organs
US20100316705A1 (en)*1999-04-142010-12-16Lauren BrasileSystem for exsanguinous metabolic support of an organ or tissue
US6582953B2 (en)*1999-04-142003-06-24Breonics, Inc.Organ chamber for exsanguinous metabolic support system
US6345962B1 (en)*2000-05-222002-02-12Douglas E. SutterFluid operated pump
US8323954B2 (en)2000-08-252012-12-04Lifeline Scientific, Inc.Apparatus and method for maintaining and/or restoring viability of organs
US20110183310A1 (en)*2000-08-252011-07-28Lifeline Scientific, Inc.Apparatus and method for maintaining and/or restoring viability of organs
US7326564B2 (en)2001-02-202008-02-05St. Jude Medical, Inc.Flow system for medical device evaluation and production
WO2002089571A1 (en)*2001-05-042002-11-14Breonics, Inc.Organ chamber for exsanguinous metabolic support system
US20040221719A1 (en)*2003-04-042004-11-11Organ Recovery Systems, Inc.Device for separating gas from a liquid path
US20100151559A1 (en)*2003-04-042010-06-17Lifeline Scientific, Inc.Method and apparatus for transferring heat to or from an organ or tissue container
US8389271B2 (en)2003-04-042013-03-05Organ Recovery Systems, Inc.Method and apparatus for controlling air pressure in an organ or tissue container
US7678563B2 (en)2003-04-042010-03-16Organ Recovery Systems, Inc.Method and apparatus for controlling air pressure in an organ or tissue container
US7998725B2 (en)2003-04-042011-08-16Organ Recovery SystemsMethod and apparatus for holding a plurality of tubes connectible to an organ or tissue container
US20100112542A1 (en)*2003-04-042010-05-06Organ Recovery Systems, Inc.Method and apparatus for controlling air pressure in an organ or tissue container
US8128740B2 (en)2003-04-042012-03-06Organ Recovery Systems, Inc.Device for separating gas from a liquid path
US20040235142A1 (en)*2003-04-042004-11-25Organ Recovery SystemsMethod and apparatus for holding a plurality of tubes connectible to an organ or tissue container
US20040224299A1 (en)*2003-04-042004-11-11Organ Recovery SystemsMethod and apparatus for transferring heat to or from an organ or tissue container
US7691622B2 (en)2003-04-042010-04-06Lifeline Scientific, Inc.Method and apparatus for transferring heat to or from an organ or tissue container
US8097449B2 (en)2003-04-042012-01-17Organ Recovery SystemsMethod and apparatus for transferring heat to or from an organ or tissue container
US7897327B2 (en)2003-06-022011-03-01Organ Recovery Systems, Inc.Method and apparatus for pressure control for maintaining viability of organs
US20040241634A1 (en)*2003-06-022004-12-02Organ Recovery SystemsMethod and apparatus for pressure control for maintaining viability of organs
WO2004110146A1 (en)*2003-06-022004-12-23Organ Recovery Systems, Inc.Method and apparatus for pressure control for maintaining viability of organs
US20050221269A1 (en)*2004-04-052005-10-06Organ Recovery SystemsApparatus and method for perfusing an organ or tissue for isolating cells from the organ or tissue
US20090226878A1 (en)*2004-04-052009-09-10Organ Recovery SystemsApparatus and method for perfusing an organ or tissue for isolating cells from the organ or tissue
US9706769B2 (en)2004-04-052017-07-18Organ Recovery Systems, IncApparatus and method for maintaining and/or restoring viability of organs
US7504201B2 (en)2004-04-052009-03-17Organ Recovery SystemsMethod for perfusing an organ and for isolating cells from the organ
US8389280B2 (en)2004-04-052013-03-05Organ Recovery SystemsMethod for perfusing an organ for isolating cells from the organ
US9055740B2 (en)2004-10-072015-06-16Transmedics, Inc.Systems and methods for ex-vivo organ care
US20060154357A1 (en)*2004-10-072006-07-13Transmedics, Inc.Systems and methods for ex-vivo organ care
US10321676B2 (en)2004-10-072019-06-18Transmedics, Inc.System and methods for ex-vivo organ care and for using lactate as an indication of donor organ status
US12010987B2 (en)2004-10-072024-06-18Transmedics, Inc.Systems and methods for ex-vivo organ care and for using lactate as an indication of donor organ status
US9894894B2 (en)2004-10-072018-02-20Transmedics, Inc.Systems and methods for ex-vivo organ care and for using lactate as an indication of donor organ status
US10736314B2 (en)2004-10-072020-08-11Transmedics, Inc.Systems and methods for ex-vivo organ care and for using lactate as an indication of donor organ status
US20060148062A1 (en)*2004-10-072006-07-06Transmedics, Inc.Systems and methods for ex-vivo organ care
US11570985B2 (en)2004-10-072023-02-07Transmedics, Inc.Systems and methods for ex-vivo organ care and for using lactate as an indication of donor organ status
US12396454B2 (en)2004-10-072025-08-26Transmedics, Inc.Systems and methods for ex-vivo organ care and for using lactate as an indication of donor organ status
US9301519B2 (en)2004-10-072016-04-05Transmedics, Inc.Systems and methods for ex-vivo organ care
US11191263B2 (en)2004-10-072021-12-07Transmedics, Inc.Systems and methods for ex-vivo organ care
US12137683B2 (en)2004-10-072024-11-12Transmedics, Inc.Systems and methods for ex-vivo organ care
US9215867B2 (en)2004-10-072015-12-22Transmedics, Inc.Systems and methods for ex-vivo organ care
US10314303B2 (en)2004-10-072019-06-11Transmedics, Inc.Systems and methods for ex-vivo organ care
US11723357B2 (en)2004-10-072023-08-15Transmedics, Inc.Systems and methods for ex-vivo organ care
US20130217128A1 (en)*2005-02-172013-08-22Technische Universiteit EindhovenMethod of manufacturing a tissue-engineered prosthesis
US9078428B2 (en)2005-06-282015-07-14Transmedics, Inc.Systems, methods, compositions and solutions for perfusing an organ
US11844345B2 (en)2005-06-282023-12-19Transmedics, Inc.Systems, methods, compositions and solutions for perfusing an organ
US10039276B2 (en)2005-06-282018-08-07Transmedics, Inc.Systems, methods, compositions and solutions for perfusing an organ
US8470520B2 (en)2005-08-262013-06-25Regents Of The University Of MinnesotaDecellularization and recellularization of organs and tissues
US10220056B2 (en)2005-08-262019-03-05Miromatrix Medical, Inc.Decellularization and recellularization of solid organs
US20090202977A1 (en)*2005-08-262009-08-13Regents Of The University Of MinnesotaDecellularization and recellularization of organs and tissues
US10441609B2 (en)2005-08-262019-10-15Miromatrix Medical Inc.Decellularization and recellularization of solid organs
US20100093066A1 (en)*2005-08-262010-04-15Regents Of The University Of MinnesotaDecellularization and recellularization apparatuses and systems containing the same
US20110136096A1 (en)*2006-04-192011-06-09Transmedics, Inc.Systems and Methods for Ex Vivo Organ Care
US8822203B2 (en)2006-04-192014-09-02Transmedics, Inc.Systems and methods for ex vivo organ care
US12207649B2 (en)2007-03-202025-01-28Transmedics, Inc.Systems for monitoring and applying electrical currents in an organ perfusion system
US10327443B2 (en)2007-03-202019-06-25Transmedics, Inc.Systems for monitoring and applying electrical currents in an organ perfusion system
US9457179B2 (en)2007-03-202016-10-04Transmedics, Inc.Systems for monitoring and applying electrical currents in an organ perfusion system
US11917991B2 (en)2007-03-202024-03-05Transmedics, Inc.Systems for monitoring and applying electrical currents in an organ perfusion system
US20080234768A1 (en)*2007-03-202008-09-25Transmedics, IncSystems for monitoring and applying electrical currents in an organ perfusion system
US20110003275A1 (en)*2007-07-062011-01-06Igelosa Transplantation Science AbSystem and method for organ evaluation and preservation
WO2009020412A1 (en)*2007-07-062009-02-12Xenodevice AbSystem and method for organ evaluation and preservation
US20090197292A1 (en)*2008-01-312009-08-06Transmedics, IncSystems and methods for ex vivo lung care
US9814230B2 (en)2008-01-312017-11-14Transmedics, Inc.Systems and methods for ex vivo lung care
US20090197325A1 (en)*2008-01-312009-08-06Transmedics, IncSYSTEMS AND METHODS FOR Ex vivo LUNG CARE
US12317888B2 (en)2008-01-312025-06-03Transmedics, IncSystems and methods for ex vivo lung care
US20090197240A1 (en)*2008-01-312009-08-06Transmedics, IncSystems and methods for ex vivo lung care
US9516875B2 (en)2008-01-312016-12-13Transmedics, Inc.Systems and methods for ex vivo lung care
US9462802B2 (en)2008-01-312016-10-11Transmedics, Inc.Systems and methods for ex vivo lung care
US10750738B2 (en)2008-01-312020-08-25Transmedics, Inc.Systems and methods for ex vivo lung care
US9247728B2 (en)2008-01-312016-02-02Transmedics, Inc.Systems and methods for ex vivo lung care
EP2318066A4 (en)*2008-08-012018-03-28Biomedinnovations, LlcMethods and apparatus for organ support
US9089126B2 (en)*2008-08-012015-07-28Biomedinnovations, LlcMethods and apparatus for organ support
US20100028979A1 (en)*2008-08-012010-02-04Faulkner Donald GMethods and apparatus for organ support
US8329450B2 (en)*2008-08-012012-12-11Biomedinnovations, LlcMethods and apparatus for organ support
WO2010014928A2 (en)2008-08-012010-02-04Biomedinnovations, LlcMethods and apparatus for organ support
US20110104651A1 (en)*2009-11-042011-05-05Sweeney Terrence EMechanical Model of the Cardiovascular System and Method of Demonstrating the Physiology of the Cardiovascular System
US9881523B2 (en)2009-11-042018-01-30University Of ScrantonMechanical model of the cardiovascular system and method of demonstrating the physiology of the cardiovascular system
US9576504B2 (en)*2009-11-042017-02-21University Of ScrantonMechanical model of the cardiovascular system and method of demonstrating the physiology of the cardiovascular system
US9974897B2 (en)*2010-01-132018-05-22Hemovent GmbhArrangement with a blood pump and a gas exchanger for extracorporeal membrane oxygenation
US20130004369A1 (en)*2010-01-132013-01-03Oliver MarseilleArrangement with a blood pump and a gas exchanger for extracorporeal membrane oxygenation
US11173238B2 (en)2010-01-132021-11-16Hemovent GmbhArrangement with a blood pump and a gas exchanger for extracorporeal membrane oxygenation
US8882695B2 (en)*2010-01-132014-11-11Mecora Medizintechnik GmbhArrangement with a blood pump and a gas exchanger for extracorporeal membrane oxygenation
US20150025448A1 (en)*2010-01-132015-01-22Mecora Medizintechnik GmbhArrangement with a blood pump and a gas exchanger for extracorporeal membrane oxygenation
US12084677B2 (en)2010-09-012024-09-10Regents Of The University Of MinnesotaMethods of recellularizing a tissue or organ for improved transplantability
US10233420B2 (en)2010-09-012019-03-19Regents Of The University Of MinnesotaMethods of recellularizing a tissue or organ for improved transplantability
US11414644B2 (en)2010-09-012022-08-16Regents Of The University Of MinnesotaMethods of recellularizing a tissue or organ for improved transplantability
US11856944B2 (en)2011-04-142024-01-02Transmedics, Inc.Organ care solution for ex-vivo machine perfusion of donor lungs
US20140135697A1 (en)*2011-06-202014-05-15Veinux ApsDisposable heat exchange cassette and an assembly for heating intravenous fluid
US9290738B2 (en)2012-06-132016-03-22Miromatrix Medical Inc.Methods of decellularizing bone
US11452797B2 (en)2013-03-152022-09-27Miromatrix Medical Inc.Use of perfusion decellularized liver for islet cell recellularization
US10076112B2 (en)2014-06-022018-09-18Transmedic, Inc.Ex vivo organ care system
US11903381B2 (en)2014-06-022024-02-20Transmedics, Inc.Ex vivo organ care system
US11944088B2 (en)2014-06-022024-04-02Transmedics, Inc.Ex vivo organ care system
US11154050B2 (en)2014-06-022021-10-26Transmedics, Inc.Ex vivo organ care system
US11963526B2 (en)2014-12-122024-04-23Transmedics, Inc.Apparatus and method for organ perfusion
US12185718B2 (en)2015-09-092025-01-07Transmedics, Inc.Aortic cannula for ex vivo organ care system
US11122795B2 (en)2015-09-092021-09-21Transmedics, Inc.Aortic cannula for ex vivo organ care system
US10194655B2 (en)2015-09-092019-02-05Transmedics, Inc.Aortic cannula for ex vivo organ care system
US12127554B2 (en)2016-05-302024-10-29Transmedics, Inc.Apparatus and method for ex vivo lung ventilation with a varying exterior pressure
US12076461B2 (en)2016-09-062024-09-03Miromatrix Medical Inc.Use of resected liver serum for whole liver-engineering
US11278643B2 (en)2016-09-062022-03-22Mayo Foundation For Medical Education And ResearchUse of resected liver serum for whole liver-engineering
US12280192B2 (en)2017-09-202025-04-22Hemovent GmbhGas exchange unit
US12263275B2 (en)2018-06-132025-04-01Miromatrix Medical Inc.Fistula filler and deployment system
US12115284B1 (en)2021-06-092024-10-15Reprise Biomedical, Inc.Biologic matrix for a wound site and related methods
US11998662B1 (en)2021-06-092024-06-04Reprise Biomedical, Inc.Biologic matrix for a wound site and related methods
US12383657B1 (en)2021-06-092025-08-12Reprise Biomedical, Inc.Biologic matrix for a wound site and related methods

Also Published As

Publication numberPublication date
GB1343728A (en)1974-01-16
AU2618871A (en)1972-09-07
ZA711359B (en)1971-12-29
BE764090A (en)1971-08-02
FR2092431A5 (en)1972-01-21
DE2115333A1 (en)1971-10-21

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