Ventricular assist device: Difference between revisions
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{{Short description|Medical device to assist or replace a heart}} |
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{{Use dmy dates|date=August 2021}} |
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| Name = Ventricular assist device |
| Name = Ventricular assist device |
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| Image = Ventricular assist device.png |
| Image = Ventricular assist device.png |
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| Caption = A left ventricular assist device (LVAD) pumping blood from the left ventricle to the aorta, connected to an externally worn control unit and battery pack. |
| Caption = A left ventricular assist device (LVAD) pumping blood from the left ventricle to the aorta, connected to an externally worn control unit and battery pack. |
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| MedlinePlus = 007268 |
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A '''ventricular assist device''' ('''VAD''') is an [[electromechanics|electromechanical]] device that provides support for cardiac pump function, which is used either to partially or to completely replace the function of a failing [[heart]]. VADs can be used in patients with acute (sudden onset) or chronic (long standing) [[heart failure]], which can occur due to [[coronary artery disease]], [[atrial fibrillation]], [[valvular disease]], and other conditions.<ref>{{Cite journal |last1=Savarese |first1=Gianluigi |last2=Becher |first2=Peter Moritz |last3=Lund |first3=Lars H. |last4=Seferovic |first4=Petar |last5=Rosano |first5=Giuseppe M. C. |last6=Coats |first6=Andrew J. S. |date=2023-01-18 |title=Global burden of heart failure: a comprehensive and updated review of epidemiology |journal=Cardiovascular Research |volume=118 |issue=17 |pages=3272–3287 |doi=10.1093/cvr/cvac013 |issn=1755-3245 |pmid=35150240|doi-access=free }}</ref><ref>{{Cite journal |last1=Kirkpatrick |first1=James N. |last2=Wieselthaler |first2=Georg |last3=Strueber |first3=Martin |last4=St John Sutton |first4=Martin G. |last5=Rame |first5=J. Eduardo |date=July 2015 |title=Ventricular assist devices for treatment of acute heart failure and chronic heart failure |url=https://pubmed.ncbi.nlm.nih.gov/25948420 |journal=Heart (British Cardiac Society) |volume=101 |issue=14 |pages=1091–1096 |doi=10.1136/heartjnl-2014-306789 |issn=1468-201X |pmid=25948420|s2cid=6958416 }}</ref> |
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A '''ventricular assist device (VAD)''' is an [[electromechanics|electromechanical]] device for assisting cardiac circulation, which is used either to partially or to completely replace the function of a failing [[heart]]. The function of VADs is different from that of [[artificial cardiac pacemaker]]s; some are for short-term use, typically for patients recovering from [[myocardial infarction]] (heart attack) and for patients recovering from [[cardiac surgery]]; some are for long-term use (months to years to perpetuity), typically for patients suffering from advanced [[heart failure]]. |
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==Categorization of VADs== |
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VADs are designed to assist either the right [[ventricle (heart)|ventricle]] (RVAD) or the left ventricle (LVAD), or to assist both ventricles (BiVAD). The type of ventricular assistance device applied depends upon the type of underlying [[heart disease]], and upon the pulmonary arterial resistance, which determines the workload of the right ventricle. The left ventricle assistance device (LVAD) is the most common device applied to a defective heart (it is sufficient in most cases; the right side of the heart is then often able to make use of the heavily increased blood flow), but when the pulmonary arterial resistance is high, then an (additional) right ventricle assistance device (RVAD) might be necessary to resolve the problem of cardiac circulation. If both a LVAD and a RVAD is needed a BiVAD is normally used, rather than a separate LVAD and an RVAD. |
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VADs may be used to manage a variety of cardiac diseases and can be categorized based on which ventricle the device is assisting, and whether the VAD will be temporary or permanent. |
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'''Ventricular Assistance''' |
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Normally, the long-term VAD is used as a [[bridge to transplantation]] (BTT)—keeping the patient alive, and in reasonably good condition, and able to await the heart transplant outside of the hospital. |
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Other "bridges" include bridge to candidacy, bridge to decision, and bridge to recovery. |
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In some instances VADs are also used as [[destination therapy]] (DT). In this instance, the patient shall not undergo a heart transplantion and the VAD is what the patient will use for the remainder of their life.<ref name="content.nejm.org">{{Cite journal| last1 = Birks | first1 = EJ| last2 = Tansley | first2 = PD | last3 = Hardy | first3 = J|display-authors=etal | doi = 10.1056/NEJMoa053063 | title = Left Ventricular Assist Device and Drug Therapy for the Reversal of Heart Failure | journal = [[New England Journal of Medicine]] | volume = 355 | issue = 18 | pages = 1873–1884 | year = 2006 | pmid = 17079761 }}</ref><ref name="ventracor.com">[https://web.archive.org/web/20080204022437/http://www.ventracor.com/news_item.asp?newsID=431 "First VentrAssist Heart Recovery Featured on National TV"]. ''Ventracor.com''. 19 October 2006.</ref> |
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First, VADs can be categorized based on whether they are designed to assist the right [[ventricle (heart)|ventricle]] (RVAD) or the left ventricle (LVAD) or to both ventricles (BiVAD). The type of VAD implanted depends on the type of underlying [[heart disease]] (e.g. patients with right ventricular failure from [[pulmonary arterial hypertension]] may require an RVAD, versus those with left ventricular failure from a [[myocardial infarction]] may require an LVAD). The LVAD is the most common device applied to a defective heart (it is sufficient in most cases; the right side of the heart is then often able to make use of the heavily increased blood flow), but when the pulmonary arterial resistance is high, then an (additional) right ventricular assist device (RVAD) might be necessary to resolve the problem of cardiac circulation. If both an LVAD and an RVAD are needed a BiVAD is normally used, rather than a separate LVAD and RVAD.{{cn|date=November 2023}} |
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VADs are distinct from [[artificial heart]]s, which are designed to assume cardiac function, and generally require the removal of the patient's heart. |
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'''Duration''' |
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VADs can further be divided by the duration of their use (i.e. temporary versus permanent). Some VADs are for short-term use,<ref>{{cite journal |last1=Sef |first1=D |last2=Mohite |first2=P |last3=De Robertis |first3=F |last4=Verzelloni Sef |first4=A |last5=Mahesh |first5=B |last6=Stock |first6=U |last7=Simon |first7=A |date=September 2020 |title=Bridge to heart transplantation using the Levitronix CentriMag short-term ventricular assist device. |journal=Artificial Organs |volume=44 |issue=9 |pages=1006–1008 |doi=10.1111/aor.13709 |pmid=32367538 |s2cid=218506853}}</ref> typically for patients recovering from [[myocardial infarction]] (heart attack) and for patients recovering from [[cardiac surgery]]; some are for long-term use (months to years to perpetuity), typically for patients with advanced [[heart failure]]{{cn|date=November 2023}} |
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Temporary use of VADs may vary in scale (e.g. days to months) depending on a patient's condition. Certain types of VADS may be used in patients with signs of acute (sudden onset) heart failure or cardiogenic shock as a result of an infarction, valvular disease, among other causes.<ref>{{Cite journal |last1=Balthazar |first1=Tim |last2=Vandenbriele |first2=Christophe |last3=Verbrugge |first3=Frederik H. |last4=Den Uil |first4=Corstiaan |last5=Engström |first5=Annemarie |last6=Janssens |first6=Stefan |last7=Rex |first7=Steffen |last8=Meyns |first8=Bart |last9=Van Mieghem |first9=Nicolas |last10=Price |first10=Susanna |last11=Adriaenssens |first11=Tom |date=2021-03-09 |title=Managing Patients With Short-Term Mechanical Circulatory Support: JACC Review Topic of the Week |journal=Journal of the American College of Cardiology |volume=77 |issue=9 |pages=1243–1256 |doi=10.1016/j.jacc.2020.12.054 |issn=1558-3597 |pmid=33663742|s2cid=232123771 |doi-access=free |hdl=1942/34157 |hdl-access=free }}</ref> In patients with acute signs of heart failure, small [[percutaneous]] (introduced to the heart through the skin into a blood vessel rather than through an incision) VADs such as the [[Impella]] 5.5, Impella RP, and others can be introduced to either the left or right ventricle (depending on the patient-specific needs) using a wire and that is introduced through the arteries or veins of the neck, axilla, or groin.<ref>{{Cite web |title=Impella 5.5® with SmartAssist®{{!}} Product {{!}} Healthcare Professionals |url=https://www.heartrecovery.eu/products-and-services/impella/impella-55-with-smartassist |access-date=2023-10-26 |website=www.heartrecovery.eu |language=en}}</ref> |
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Long-term use of VADs may also vary in its scale (i.e. months to permanently). VADs that are intended for long term use are also termed "durable" VADS, due to their design to function for longer periods of time compared to short term VADs (e.g. Impella, etc.). The long-term VADs can be used in a variety of scenarios. First, VADs may be used as [[bridge to transplantation]] (BTT) – keeping the patient alive, and in reasonably good condition, and able to await heart transplant outside of the hospital. Other "bridges" include bridge to candidacy (used when a patient has a [[contraindication]] to heart transplantation but is expected to improve with the VADs support) , bridge to decision (used to support a patient while their candidacy status is decided), and bridge to recovery (used until a patient’s native heart function improves after which the device would be removed).<ref>{{Cite journal |last=Frigerio |first=Maria |date=October 2021 |title=Left Ventricular Assist Device: Indication, Timing, and Management |url=https://pubmed.ncbi.nlm.nih.gov/34511210 |journal=Heart Failure Clinics |volume=17 |issue=4 |pages=619–634 |doi=10.1016/j.hfc.2021.05.007 |issn=1551-7136 |pmid=34511210}}</ref> In some instances, VADs are also used as [[destination therapy]] (DT) which indicates that the VAD will remain implanted indefinitely. VADs as destination therapy are used in circumstances where patients are not candidates for transplantation and will thus rely on the VAD for the remainder of their life.<ref name="content.nejm.org">{{Cite journal| last1 = Birks | first1 = EJ| last2 = Tansley | first2 = PD | last3 = Hardy | first3 = J|display-authors=etal | doi = 10.1056/NEJMoa053063 | title = Left Ventricular Assist Device and Drug Therapy for the Reversal of Heart Failure | journal = [[New England Journal of Medicine]] | volume = 355 | issue = 18 | pages = 1873–1884 | year = 2006 | pmid = 17079761 | doi-access = free }}</ref><ref name="ventracor.com">[https://web.archive.org/web/20080204022437/http://www.ventracor.com/news_item.asp?newsID=431 "First VentrAssist Heart Recovery Featured on National TV"]. ''Ventracor.com''. 19 October 2006.</ref> |
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'''Other Cardiac Support Devices''' |
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Some devices are designed to support the heart and its various components/function but are not considered VADs, below are some common examples. |
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[[Pacemakers]] and Internal Cardiac Defibrillators (ICDs) – the function of a VAD differs from that of an [[artificial cardiac pacemaker]] in that a VAD pumps [[blood]], whereas a pacemaker delivers electrical impulses to the heart muscle. |
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Total Artificial Heart – VADs are distinct from [[artificial heart]]s, which are designed to assume cardiac function, and generally require the removal of the patient's heart.<ref>{{Cite journal |last1=Chung |first1=Joshua S. |last2=Emerson |first2=Dominic |last3=Megna |first3=Dominick |last4=Arabia |first4=Francisco A. |date=March 2020 |title=Total artificial heart: surgical technique in the patient with normal cardiac anatomy |journal=Annals of Cardiothoracic Surgery |volume=9 |issue=2 |pages=81–88 |doi=10.21037/acs.2020.02.09 |issn=2225-319X |pmc=7160624 |pmid=32309155 |doi-access=free }}</ref> |
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Extracorporeal Membrane Oxygenation (ECMO) – is a form of mechanical circulatory support typically used in critically ill patients in cardiogenic shock that is established by introducing cannula into the arteries and or veins of the neck, axilla or groin. Generally, a venous cannula pulls deoxygenated blood from the patient's veins into an oxygenating device at the patient's bedside, after which a motor powered pump moves the oxygenated blood is back to the body (either into a vein or the arterial system, typically the aorta). There are different ECMO configurations (venoarterial ECMO, venovenous ECMO, etc.) the end goal remains the same; to oxygenate blood and return it to the body.<ref>{{Cite journal |last1=Vieira |first1=Jefferson L. |last2=Ventura |first2=Hector O. |last3=Mehra |first3=Mandeep R. |date=2020 |title=Mechanical circulatory support devices in advanced heart failure: 2020 and beyond |url=https://pubmed.ncbi.nlm.nih.gov/32971112 |journal=Progress in Cardiovascular Diseases |volume=63 |issue=5 |pages=630–639 |doi=10.1016/j.pcad.2020.09.003 |issn=1873-1740 |pmid=32971112|s2cid=221917384 }}</ref> In this sense, the ECMO circuit bypasses one or both ventricles and is therefore not in contact with the patient's native ventricle and is generally not considered a type of VAD. |
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==Design== |
==Design== |
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===Pumps=== |
===Pumps=== |
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The [[pump]]s used in VADs can be divided into two main |
The [[pump]]s used in VADs can be divided into two main categories – pulsatile pumps,<ref>{{cite book|last1=Fajdek|first1=B|last2=Krzysztof|first2=J|title=2014 19th International Conference on Methods and Models in Automation and Robotics (MMAR)|chapter=Automatic control system for ventricular assist device|date=2–5 September 2014|pages=874–879|doi=10.1109/MMAR.2014.6957472|isbn=978-1-4799-5081-2|s2cid=13070912}}</ref> which mimic the natural pulsing action of the heart, and continuous-flow pumps.<ref>{{Cite journal | last1 = Schulman | first1 = AR | last2 = Martens | first2 = TP | last3 = Christos | first3 = PJ|display-authors=etal |
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| doi = 10.1016/j.jtcvs.2006.09.083 | first10 = S. H. | title = Comparisons of infection complications between continuous flow and pulsatile flow left ventricular assist devices | journal = [[The Journal of Thoracic and Cardiovascular Surgery]] | volume = 133 | issue = 3 | pages = 841–842 | year = 2007 | pmid = 17320612 }}</ref> Pulsatile VADs use [[positive displacement pump]]s.<ref>{{cite web|url=https://openi.nlm.nih.gov/detailedresult.php?img=PMC3303031_12471_2011_211_Fig2_HTML&req=4|title=Panel A shows a first-generation pulsatile flow left ve - Open-i |
| doi = 10.1016/j.jtcvs.2006.09.083 | first10 = S. H. | title = Comparisons of infection complications between continuous flow and pulsatile flow left ventricular assist devices | journal = [[The Journal of Thoracic and Cardiovascular Surgery]] | volume = 133 | issue = 3 | pages = 841–842 | year = 2007 | pmid = 17320612 | doi-access = free }}</ref> Pulsatile VADs use [[positive displacement pump]]s.<ref>{{cite web|url=https://openi.nlm.nih.gov/detailedresult.php?img=PMC3303031_12471_2011_211_Fig2_HTML&req=4|title=Panel A shows a first-generation pulsatile flow left ve - Open-i|website=openi.nlm.nih.gov|access-date=23 April 2018}}</ref><ref name="j785">{{cite journal | last=Ruden | first=Serena A. S. Von | last2=Murray | first2=Margaret A. | last3=Grice | first3=Jennifer L. | last4=Proebstle | first4=Amy K. | last5=Kopacek | first5=Karen J. | title=The Pharmacotherapy Implications of Ventricular Assist Device in the Patient With End-Stage Heart Failure | journal=Journal of Pharmacy Practice | volume=25 | issue=2 | date=2012 | issn=0897-1900 | doi=10.1177/0897190011431635 | pages=232–249}}</ref><ref>{{cite web|url=http://www.syncardia.com/dldir1/8263_C026.pdf|title=SynCardia TAH pulsatile pump components|website=syncardia.com|access-date=23 April 2018}}</ref> In some pulsatile pumps (that use compressed air as an energy source<ref>{{cite web|url=http://www.aldmd.com/cards2_assets/Heartmate%20XVE.pdf|title=The HeartMate XVE too has a vent line, despite being battery-powered|website=aldmd.com|access-date=23 April 2018}}</ref>), the volume occupied by blood varies during the pumping cycle. If the pump is contained inside the body then a vent tube to the outside air is required. |
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Continuous-flow VADs are smaller and have proven to be more durable than pulsatile VADs.<ref>{{Cite journal | last1 = Slaughter | first1 = MS | last2 = Pagani | first2 = FD | last3 = Rogers | first3 = JG|display-authors=etal | doi = 10.1016/j.healun.2010.01.011 | title = Clinical management of continuous-flow left ventricular assist devices in advanced heart failure | journal = The Journal of Heart and Lung Transplantation | volume = 29 | issue = 4 | pages = S1–39 | year = 2010 | pmid = 20181499 }}</ref> They normally use either a [[centrifugal pump]] or an [[axial flow pump]]. Both types have a central rotor containing permanent magnets. Controlled electric currents running through coils contained in the pump housing apply forces to the magnets, which in turn cause the rotors to spin. In the centrifugal pumps, the rotors are shaped to accelerate the blood circumferentially and thereby cause it to move toward the outer rim of the pump, whereas in the axial flow pumps the rotors are more or less cylindrical with blades that are helical, causing the blood to be accelerated in the direction of the rotor's axis.<ref name=fukamachi_2005>{{cite journal |last= Fukamachi |first= Kiyo |author2=Smedira, Nicholas |date=August 2005 |title= Smaller, Safer, Totally Implantable LVADs: Fact or Fantasy?|journal= |
Continuous-flow VADs are smaller and have proven to be more durable than pulsatile VADs.<ref>{{Cite journal | last1 = Slaughter | first1 = MS | last2 = Pagani | first2 = FD | last3 = Rogers | first3 = JG|display-authors=etal | doi = 10.1016/j.healun.2010.01.011 | title = Clinical management of continuous-flow left ventricular assist devices in advanced heart failure | journal = The Journal of Heart and Lung Transplantation | volume = 29 | issue = 4 | pages = S1–39 | year = 2010 | pmid = 20181499 }}</ref> They normally use either a [[centrifugal pump]] or an [[axial flow pump]]. Both types have a central rotor containing permanent magnets. Controlled electric currents running through coils contained in the pump housing apply forces to the magnets, which in turn cause the rotors to spin. In the centrifugal pumps, the rotors are shaped to accelerate the blood circumferentially and thereby cause it to move toward the outer rim of the pump, whereas in the axial flow pumps the rotors are more or less cylindrical with blades that are helical, causing the blood to be accelerated in the direction of the rotor's axis.<ref name=fukamachi_2005>{{cite journal |last= Fukamachi |first= Kiyo |author2=Smedira, Nicholas |date=August 2005 |title= Smaller, Safer, Totally Implantable LVADs: Fact or Fantasy?|journal= ACC Current Journal Review |volume= 14 |issue= 8 |pages= 40–42 |doi=10.1016/j.accreview.2005.06.001}}</ref> |
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An important issue with continuous flow pumps is the method used to suspend the rotor. Early versions used solid bearings; however, newer pumps, some of which are approved for use in the EU, use either [[magnetic levitation]] ("maglev")<ref>Smart, Frank. [http://www.healio.com/cardiology/hf-transplantation/news/print/cardiology-today/%7B74b7c676-ca44-4c7c-9d9b-ed4f84a33e27%7D/magnetic-levitation-heart-pump-implanted-in-first-us-patient "Magnetic levitation heart pump implanted in first U.S. patient"]. "Cardiology Today". October 2008.</ref><ref>{{Cite journal | last1 = Pai | first1 = CN | last2 = Shinshi | first2 = T | last3 = Asama | first3 = J|display-authors=etal | title = Development of a Compact Maglev Centrifugal Blood Pump Enclosed in a Titanium Housing | doi = 10.1299/jamdsm.2.343 | journal = Journal of Advanced Mechanical Design, Systems, and Manufacturing | volume = 2 | issue = 3 | pages = 343–355 | year = 2008 | |
An important issue with continuous flow pumps is the method used to suspend the rotor. Early versions used solid bearings; however, newer pumps, some of which are approved for use in the EU, use either [[magnetic levitation]] ("maglev")<ref>Smart, Frank. [http://www.healio.com/cardiology/hf-transplantation/news/print/cardiology-today/%7B74b7c676-ca44-4c7c-9d9b-ed4f84a33e27%7D/magnetic-levitation-heart-pump-implanted-in-first-us-patient "Magnetic levitation heart pump implanted in first U.S. patient"]. "Cardiology Today". October 2008.</ref><ref>{{Cite journal | last1 = Pai | first1 = CN | last2 = Shinshi | first2 = T | last3 = Asama | first3 = J|display-authors=etal | title = Development of a Compact Maglev Centrifugal Blood Pump Enclosed in a Titanium Housing | doi = 10.1299/jamdsm.2.343 | journal = Journal of Advanced Mechanical Design, Systems, and Manufacturing | volume = 2 | issue = 3 | pages = 343–355 | year = 2008 | bibcode = 2008JAMDS...2..343P | doi-access = free }}</ref><ref>{{Cite journal |
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| last1 = Hoshi | first1 = H | last2 = Shinshi | first2 = T | last3 = Takatani | first3 = S | doi = 10.1111/j.1525-1594.2006.00222.x | title = Third-generation Blood Pumps with Mechanical Noncontact Magnetic Bearings | journal = Artificial Organs | volume = 30 | issue = 5 | pages = 324–338 | year = 2006 | pmid = 16683949 }}</ref> or [[fluid dynamic bearings|hydrodynamic suspension]] |
| last1 = Hoshi | first1 = H | last2 = Shinshi | first2 = T | last3 = Takatani | first3 = S | doi = 10.1111/j.1525-1594.2006.00222.x | title = Third-generation Blood Pumps with Mechanical Noncontact Magnetic Bearings | journal = Artificial Organs | volume = 30 | issue = 5 | pages = 324–338 | year = 2006 | pmid = 16683949 }}</ref> or [[fluid dynamic bearings|hydrodynamic suspension]]. |
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==History== |
==History== |
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[[File:1966 DeBakey ventricular assist device.jpg|thumb|120px|1966 DeBakey ventricular assist device.<ref><!--Reference for image only-->{{cite news|title=Dr. Denton Cooley and Dr. Michael E. DeBakey: Rock stars of Houston medicine|url=http://www.chron.com/news/health/slideshow/Dr-Denton-Cooley-and-Dr-Michael-E-DeBakey-83220/photo-6114896.php|work=[[Houston Chronicle]]|date=3 April 2014}}</ref>]] |
[[File:1966 DeBakey ventricular assist device.jpg|thumb|120px|1966 DeBakey ventricular assist device.<ref><!--Reference for image only-->{{cite news|title=Dr. Denton Cooley and Dr. Michael E. DeBakey: Rock stars of Houston medicine|url=http://www.chron.com/news/health/slideshow/Dr-Denton-Cooley-and-Dr-Michael-E-DeBakey-83220/photo-6114896.php|work=[[Houston Chronicle]]|date=3 April 2014}}</ref>]] |
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The first left ventricular assist device (LVAD) system was created by [[Domingo Liotta]] at Baylor College of Medicine in Houston in 1962. The first LVAD was implanted in 1963 by Liotta and E. Stanley Crawford. The first successful implantation of an LVAD was completed in 1966 by Liotta along with Dr. [[Michael E. DeBakey]]. The patient was a 37-year-old woman, and a paracorporeal (external) circuit was able to provide mechanical support for 10 days after the surgery.<ref>{{cite journal|last1=Kirklin|first1=JK|last2=Naftel|first2=DC|title=Mechanical circulatory support: registering a therapy in evolution.|journal=[[Circulation (journal)|Circulation: Heart Failure]]|date=September 2008|volume=1|issue=3|pages=200–5|pmid=19808290|doi=10.1161/circheartfailure.108.782599|pmc=3437761}}</ref> The first successful long-term implantation of an LVAD was conducted in 1988 by Dr. [[William F. Bernhard]] of [[Boston Children's Hospital]] Medical Center and Thermedics, Inc. of Woburn, MA, under a [[National Institutes of Health]] (NIH) research contract which developed HeartMate, an electronically controlled assist device. This was funded by a three-year $6.2 million contract to Thermedics and Children's Hospital, Boston, MA, from the [[National Heart, Lung, and Blood Institute]], a program of the NIH.<ref name="Children's Hospital Boston MA">{{cite journal|title=Heart Pump Progress Announced - A promising step in artificial heart technology|journal=Children's Today|date=19 March 1988|issue=March|page=1,5}}</ref> The early VADs emulated the heart by using a "pulsatile" action where blood is alternately sucked into the pump from the left ventricle then forced out into the aorta. Devices of this kind include the HeartMate IP LVAS, which was approved for use in the US by the [[Food and Drug Administration]] (FDA) in October 1994. These devices began to gain acceptance in the late 1990s as heart surgeons including [[Eric Rose]], [[O. H. Frazier]] and [[Mehmet Oz]] began popularizing the concept that patients could live outside the hospital. Media coverage of outpatients with VADs underscored these arguments.<ref>{{cite video|url= http://www.pbs.org/wgbh/nova/transcripts/2617eheart.html|title=Electric Heart|publisher=PBS}}</ref> |
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The first Left Ventricular Assist Device (LVAD) system was created by [[Domingo Liotta]] at Baylor College of Medicine in Houston in 1962. The first left ventricular assist device (LVAD) was implanted in 1963 by Liotta and E. Stanley Crawford. |
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The first successful implantation of a left ventricular assist device was completed in 1966 by Liotta along with Dr. [[Michael E. DeBakey]] to a 37-year-old woman. A paracorporeal (external) circuit was able to provide mechanical support for 10 days after the surgery.<ref>{{cite journal|last1=Kirklin|first1=JK|last2=Naftel|first2=DC|title=Mechanical circulatory support: registering a therapy in evolution.|journal=[[Circulation (journal)|Circulation: Heart Failure]]|date=September 2008|volume=1|issue=3|pages=200–5|pmid=19808290|doi=10.1161/circheartfailure.108.782599|pmc=3437761}}</ref> The first successful long-term implantation of an artificial LVAD was conducted in 1988 by Dr. [[William F. Bernhard]] of [[Boston Children's Hospital]] Medical Center and Thermedics, Inc of Woburn, MA under a National Institutes of Health (NIH) research contract which developed HeartMate, an electronically controlled assist device. This was funded by a three-year $6.2 million contract to Thermedics and Children's Hospital, Boston MA from the National Heart and Lung and Blood Institute, a program of the NIH.<ref name="Children's Hospital Boston MA">{{cite journal|title=Heart Pump Progress Announced - A promising step in artificial heart technology|journal=Children's Today|date=19 March 1988|issue=March|page=1,5}}</ref> The early VADs emulated the heart by using a "pulsatile" action where blood is alternately sucked into the pump from the left ventricle then forced out into the aorta. Devices of this kind include the HeartMate IP LVAS, which was approved for use in the US by the [[Food and Drug Administration]] (FDA) in October 1994. These devices began to gain acceptance in the late 1990s as heart surgeons including [[Eric Rose]], [[O. H. Frazier]] and [[Mehmet Oz]] began popularizing the concept that patients could live outside the hospital. Media coverage of outpatients with VADs underscored these arguments.<ref>{{cite video|url= http://www.pbs.org/wgbh/nova/transcripts/2617eheart.html|title=Electric Heart|publisher=PBS}}</ref> |
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More recent work has concentrated on continuous |
More recent work has concentrated on continuous-flow pumps, which can be roughly categorized as either centrifugal pumps or [[Axial flow pump|axial flow]] [[impeller]] driven pumps. These pumps have the advantage of greater simplicity resulting in smaller size and greater reliability. These devices are referred to as second-generation VADs. A side effect is that the user will not have a [[pulse]],<ref> |
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Dan Baum. |
Dan Baum. |
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[http://www.popsci.com/science/article/2012-02/no-pulse-how-doctors-reinvented-human-heart "No Pulse: How Doctors Reinvented the Human Heart"]. |
[http://www.popsci.com/science/article/2012-02/no-pulse-how-doctors-reinvented-human-heart "No Pulse: How Doctors Reinvented the Human Heart"]. |
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A very different approach in the early stages of development was the use of an inflatable cuff around the aorta. Inflating the cuff contracts the aorta and deflating the cuff allows the aorta to expand – in effect the aorta becomes a second left ventricle. A proposed refinement is to use the patient's skeletal muscle, driven by a [[pacemaker]], to power this device – which would make it truly self-contained. However, a similar operation ([[cardiomyoplasty]]) was tried in the 1990s with disappointing results.{{cn|date=November 2023}} |
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Third generation VADs suspend the impeller in the pump using either hydrodynamic or electromagnetic suspension, thus removing the need for bearings and reducing the number of moving parts to one.{{Citation needed|date=August 2009}} |
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At one time [[Peter Houghton]] was the longest surviving recipient of a VAD for permanent use. He received an experimental Jarvik 2000 LVAD in June 2000. Since then, he completed a 91-mile charity walk, published two books, lectured widely, hiked in the Swiss Alps and the American West, flew in an ultra-light aircraft, and traveled extensively around the world. He died of [[acute kidney injury]] in 2007 at the age of 69.<ref name="jarvik_houghton">{{cite news |title=The First Lifetime-Use Patient |url= http://www.jarvikheart.com/basic.asp?id=63 |archive-url=https://web.archive.org/web/20101121172612/http://www.jarvikheart.com/basic.asp?id=63|archive-date=21 November 2010 |publisher= Jarvik Heart}}</ref><ref name="texasheart">[https://web.archive.org/web/20080720113602/http://texasheart.org/AboutUs/News/Lucky7_device_07_06_07.cfm Patient Sets World Record for Living with Heart Assist Device]. Texas Heart Institute. 6 July 2007.</ref> Since then, patient Lidia Pluhar has exceeded Houghton's longevity on a VAD, having received a HeartMate II in March 2011 at age 75, and currently continues to use the device. In August 2007 the International Consortium of Circulatory Assist Clinicians (ICCAC) was founded by Anthony "Tony" Martin, a nurse practitioner (NP) and clinical manager of the mechanical circulatory support (MCS) program at Newark Beth Israel Medical Center, Newark, N.J. The ICCAC was developed as a 501c3 organization, dedicated to the development of best practices and education related to the care of individuals requiring MCS as a bridge to heart transplantation or as destination therapy in those individuals who don't meet the criteria for heart transplantation.<ref>{{cite web |url=https://iccac.global/ |title = Home {{!}} ICCAC}}</ref> |
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Another technology undergoing clinical trials is the use of transcutaneous induction to power and control the device rather than using percutaneous cables. Apart from the obvious cosmetic advantage this reduces the risk of infection and the consequent need to take preventative action. A pulsatile pump using this technology has CE Mark approval and is in clinical trials for US FDA approval.{{Citation needed|date=August 2009}} |
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A very different approach in the early stages of development is the use of an inflatable cuff around the aorta. Inflating the cuff contracts the aorta and deflating the cuff allows the aorta to expand—in effect the aorta becomes a second left ventricle. A proposed refinement is to use the patient's skeletal muscle, driven by a [[pacemaker]], to power this device which would make it truly self-contained. However a similar operation ([[cardiomyoplasty]]) was tried in the 1990s with disappointing results. In any case, it has substantial potential advantages in avoiding the need to operate on the heart itself and in avoiding any contact between blood and the device. This approach involves a return to a pulsatile flow.{{Citation needed|date=August 2009}} |
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[[Peter Houghton]] was the longest surviving recipient of a VAD for permanent use. He received an experimental Jarvik 2000 LVAD in June 2000. Since then, he completed a 91-mile charity walk, published two books, lectured widely, hiked in the Swiss Alps and the American West, flew in an ultra-light aircraft, and traveled extensively around the world. He died of [[acute kidney injury]] in 2007 at the age of 69.<ref name=jarvik_houghton>{{cite news |title=The First Lifetime-Use Patient |url= http://www.jarvikheart.com/basic.asp?id=63 |archiveurl=https://web.archive.org/web/20101121172612/http://www.jarvikheart.com/basic.asp?id=63|archivedate=21 November 2010 |publisher= Jarvik Heart}}</ref><ref name=texasheart>[https://web.archive.org/web/20080720113602/http://texasheart.org/AboutUs/News/Lucky7_device_07_06_07.cfm Patient Sets World Record for Living with Heart Assist Device]. Texas Heart Institute. 6 July 2007.</ref> |
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==Studies and outcomes== |
==Studies and outcomes== |
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===Recent developments=== |
===Recent developments=== |
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* In August 2007 The International Consortium of Circulatory Assist Clinicians (ICCAC) was founded by Anthony "Tony" Martin. A nurse practitioner (NP) and clinical manager of the mechanical circulatory support (MCS) program at Newark Beth Israel Medical Center, Newark, N.J.. |
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*In July 2009 in England, surgeons removed a donor heart that had been implanted in a toddler next to her native heart, after her native heart had recovered. This technique suggests mechanical assist device, such as an LVAD, can take some or all the work away from the native heart and allow it time to heal.<ref>{{cite news |first= Thomas |last= Maugh |title= Transplant shows heart's reparative capabilities |url= http://articles.latimes.com/2009/jul/14/science/sci-heart14 |newspaper= [[Los Angeles Times]]|date= 14 July 2009}}</ref> |
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* In July 2009 in England, surgeons removed a donor heart that had been implanted in a toddler next to her native heart, after her native heart had recovered. This technique suggests mechanical assist device, such as an LVAD, can take some or all the work away from the native heart and allow it time to heal.<ref>{{cite news |first= Thomas |last= Maugh |title= Transplant shows heart's reparative capabilities |url= https://www.latimes.com/archives/la-xpm-2009-jul-14-sci-heart14-story.html |newspaper= [[Los Angeles Times]]|date= 14 July 2009}}</ref> |
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*In July 2009, 18-month follow-up results from the HeartMate II Clinical Trial concluded that continuous-flow LVAD provides effective hemodynamic support for at least 18 months in patients awaiting transplantation, with improved functional status and quality of life.<ref name=jacc_jul_09>{{Cite journal | last1 = Pagani | first1 = FD | last2 = Miller | first2 = LW | last3 = Russell | first3 = SD|display-authors=etal | doi = 10.1016/j.jacc.2009.03.055 | title = Extended Mechanical Circulatory Support with a Continuous-Flow Rotary Left Ventricular Assist Device | journal = [[Journal of the American College of Cardiology]] | volume = 54 | issue = 4 | pages = 312–321 | year = 2009 | pmid = 19608028 }}</ref> |
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* In July 2009, 18-month follow-up results from the HeartMate II Clinical Trial concluded that continuous-flow LVAD provides effective hemodynamic support for at least 18 months in patients awaiting transplantation, with improved functional status and quality of life.<ref name=jacc_jul_09>{{Cite journal | last1 = Pagani | first1 = FD | last2 = Miller | first2 = LW | last3 = Russell | first3 = SD|display-authors=etal | doi = 10.1016/j.jacc.2009.03.055 | title = Extended Mechanical Circulatory Support with a Continuous-Flow Rotary Left Ventricular Assist Device | journal = [[Journal of the American College of Cardiology]] | volume = 54 | issue = 4 | pages = 312–321 | year = 2009 | pmid = 19608028 | doi-access = free }}</ref> |
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*Heidelberg University Hospital reported in July 2009 that the first HeartAssist5, known as the modern version of the DeBakey VAD, was implanted there. The HeartAssist5 weighs 92 grams, is made of titanium and plastic, and serves to pump blood from the left ventricle into the aorta.<ref>{{cite news |title=Heidelberg Cardiac Surgeons implant world’s first new DeBakey Heart Assist Device|url= http://insciences.org/article.php?article_id=6496 |archiveurl=https://web.archive.org/web/20110718113010/http://insciences.org/article.php?article_id=6496|archivedate=18 July 2011|newspaper= Insciences|date= 17 August 2009}}</ref> |
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*A phase 1 clinical trial is underway (as of August 2009), consisting of patients with coronary artery bypass grafting and patients in end-stage heart failure who have a left ventricular assist device. The trial involves testing a patch called Anginera which contains cells that secrete hormone-like growth factors stimulating other cells to grow. The patches are seeded with heart muscle cells and then implanted onto the heart with the goal of getting the muscle cells to start communicating with native tissues in a way that allows for regular contractions.<ref name=az_dstar_theregen>{{cite news |first= Dale|last= Quinn|title= VA study: heart-healing patch |url= http://www.azstarnet.com/business/303476 | |
* Heidelberg University Hospital reported in July 2009 that the first HeartAssist5, known as the modern version of the DeBakey VAD, was implanted there. The HeartAssist5 weighs 92 grams, is made of titanium and plastic, and serves to pump blood from the left ventricle into the aorta.<ref>{{cite news |title=Heidelberg Cardiac Surgeons implant world's first new DeBakey Heart Assist Device|url= http://insciences.org/article.php?article_id=6496 |archive-url=https://web.archive.org/web/20110718113010/http://insciences.org/article.php?article_id=6496|archive-date=18 July 2011|newspaper= Insciences|date= 17 August 2009}}</ref> |
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* A phase 1 clinical trial is underway (as of August 2009), consisting of patients with coronary artery bypass grafting and patients in end-stage heart failure who have a left ventricular assist device. The trial involves testing a patch called Anginera which contains cells that secrete hormone-like growth factors stimulating other cells to grow. The patches are seeded with heart muscle cells and then implanted onto the heart with the goal of getting the muscle cells to start communicating with native tissues in a way that allows for regular contractions.<ref name=az_dstar_theregen>{{cite news |first= Dale|last= Quinn|title= VA study: heart-healing patch |url= http://www.azstarnet.com/business/303476 |archive-url=https://web.archive.org/web/20090807141013/http://www.azstarnet.com/business/303476|archive-date=7 August 2009|newspaper= [[Arizona Daily Star]]|date= 4 August 2009}}</ref><ref name=ctgov_anginera>{{cite news |title= A Study of Anginera in Patients Undergoing Coronary Artery Bypass Graft (CABG) Surgery |url= http://clinicaltrials.gov/ct2/show/NCT00364390 |newspaper= ClinicalTrials.gov |publisher= U.S. National Institutes of Health |date= 27 March 2009 |access-date=15 September 2009 }}</ref> |
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* In September 2009, a New Zealand news outlet, Stuff, reported that in another 18 months to two years, a new wireless device will be ready for clinical trial that will power VADs without direct contact. If successful, this may reduce the chance of infection as a result of the power cable through the skin.<ref name=kiwi_wireless>{{cite news |first= Tim |last= Hunter |title=Meet the Kiwi bionic man |url= http://www.stuff.co.nz/manawatu-standard/business/2858757/Meet-the-Kiwi-bionic-man |newspaper= [[Manawatu Standard]]|date= 13 September 2009}}</ref> |
* In September 2009, a New Zealand news outlet, Stuff, reported that in another 18 months to two years, a new wireless device will be ready for clinical trial that will power VADs without direct contact. If successful, this may reduce the chance of infection as a result of the power cable through the skin.<ref name=kiwi_wireless>{{cite news |first= Tim |last= Hunter |title=Meet the Kiwi bionic man |url= http://www.stuff.co.nz/manawatu-standard/business/2858757/Meet-the-Kiwi-bionic-man |newspaper= [[Manawatu Standard]]|date= 13 September 2009}}</ref> |
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* The [[National Institutes of Health]] (NIH) awarded a $2.8 million grant to develop a "pulse-less" total artificial heart using two VADs by [[Micromed]], initially created by [[Michael DeBakey]] and [[George Noon]]. The grant was renewed for a second year of research in August 2009. The total artificial heart was created using two HeartAssist5 VADs, whereby one VAD pumps blood throughout the body and the other circulates blood to and from the lungs.<ref name=debakey_noon>{{cite news |title= $2.8 Million Grant Renewed for Development of "Pulse-Less" Total Artificial Heart|url= http://www.businesswire.com/portal/site/google/?ndmViewId=news_view&newsId=20090806005300&newsLang=en |work= [[BusinessWire]] |date= 6 August 2009}}</ref> |
* The [[National Institutes of Health]] (NIH) awarded a $2.8 million grant to develop a "pulse-less" total artificial heart using two VADs by [[Micromed]], initially created by [[Michael DeBakey]] and [[George Noon]]. The grant was renewed for a second year of research in August 2009. The total artificial heart was created using two HeartAssist5 VADs, whereby one VAD pumps blood throughout the body and the other circulates blood to and from the lungs.<ref name=debakey_noon>{{cite news |title= $2.8 Million Grant Renewed for Development of "Pulse-Less" Total Artificial Heart|url= http://www.businesswire.com/portal/site/google/?ndmViewId=news_view&newsId=20090806005300&newsLang=en |work= [[BusinessWire]] |date= 6 August 2009}}</ref> |
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* [[HeartWare International]] announced in August 2009 that it had surpassed 50 implants of their HeartWare Ventricular Assist System in their ADVANCE Clinical Trial, an FDA-approved IDE study. The study is to assess the system as bridge-to-transplantation for patients with end-stage heart failure. The study, Evaluation of the HeartWare LVAD System for the Treatment of Advanced Heart Failure, is a multi-center study that started in May 2009.<ref>{{cite news |title= Evaluation of the HeartWare LVAD System for the Treatment of Advanced Heart Failure |url= http://www.hopkinsmedicine.org/heart_vascular_institute/clinical_trials/mechanical_circulatory_support/heartware_lvad_system_heart_failure.html|publisher= [[Johns Hopkins Hospital]] |date= May 2009}}</ref><ref>{{cite news |title= HeartWare International Surpasses 50 Implants in the US |url= http://www.bio-medicine.org/medicine-news-1/HeartWare-International-Surpasses-50-Implants-in-the-US-54995-1/|newspaper= Bio-Medicine |date= 20 August 2009}}</ref> |
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* On 27 June 2014 Hannover Medical School in Hannover, Germany performed the first human implant of HeartMate III under the direction of Professor Axel Haverich M.D., chief of the Cardiothoracic, Transplantation and Vascular Surgery Department and surgeon Jan Schmitto, M.D., PhD<ref>{{cite news|title= Thoratec Announces First HeartMate III Human Implant And Start of CE Mark Trial|url= http://phx.corporate-ir.net/phoenix.zhtml?c=95989&p=irol-newsArticle&ID=1943285|archive-url= https://archive.today/20141007133132/http://phx.corporate-ir.net/phoenix.zhtml?c=95989&p=irol-newsArticle&ID=1943285|url-status= dead|archive-date= 7 October 2014|publisher= Thoratec Corporation|date= 20 August 2009}}</ref> |
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* On 21 January 2015 a study was published in Journal of American College of Cardiology suggesting that long-term use of LVAD may induce heart regeneration.<ref>{{cite journal | year = 2015 | title = Human Ventricular Unloading Induces Cardiomyocyte Proliferation| journal = [[Journal of the American College of Cardiology]] | volume = 65 | issue = 9| pages = 892–900 | doi = 10.1016/j.jacc.2014.12.027 | pmc = 4488905| last1 = Canseco| first1 = Diana C.| last2 = Kimura| first2 = Wataru| last3 = Garg| first3 = Sonia| last4 = Mukherjee| first4 = Shibani| last5 = Bhattacharya| first5 = Souparno| last6 = Abdisalaam| first6 = Salim| last7 = Das| first7 = Sandeep| last8 = Asaithamby| first8 = Aroumougame| last9 = Mammen| first9 = Pradeep P.A.| last10 = Sadek| first10 = Hesham A. | pmid=25618530}}</ref> |
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* Hall-of-Fame Baseball Player Rod Carew had congestive heart failure and was fitted with a HeartMate II. He struggled with wearing the equipment, so he joined efforts to help supply the most helpful wear to assist the HeartMate II and HeartMate III.<ref>{{Cite web|url=http://www.carewmedicalwear.com|title=LVAD Wear|website=carewmedicalwear.com|language=en-US}}</ref> |
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* In December 2018, two clinical cases were performed in Kazakhstan and a fully wireless LVAD system of Jarvik 2000 combine with [[Leviticus Cardio]] FiVAD (Fully Implantable Ventricular Assist Device) were implanted in humans. The [[Wireless power transfer]] technology based on technique called Coplanar Energy Transfer (CET) which is capable of transferring energy from an external transmitting coil to a small receiving coil that is implanted in the human body. In the early postoperative phase, CET operation was accomplished as expected in both patients, which powered the pump and maintained the battery charged to allow medical and nursing procedures. The [[Leviticus Cardio]] FiVAD System with wireless, coplanar energy transfer technology which ameliorates infection risk by driveline elimination while providing successful energy transmission allowing for a substantial (approximately 6 hours) unholstered support of the LVAD.<ref name=":0">{{cite news |title= First human use of a wireless coplanar energy transfer coupled with a continuous-flow left ventricular assist device.|url=https://www.jhltonline.org/article/S1053-2498(19)31346-4/fulltext?mobileUi%3D0&ust=1549469495758000&usg=AFQjCNFvPUvYgBhjFEc6AiVJiYyay8wH2w|publisher= Heart and Lung Transplantation|date=4 February 2019}}</ref> |
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* On June 3, 2021, Medtronic issued an urgent medical device notice stating that their HVAD devices should no longer be implanted due to higher rates of neurological events and mortality with the HVAD vs. other available devices <ref name=":1">{{Cite web|last=Njoku|first=Nnamdi|date=June 3, 2021|title=Urgent Medical Device Communication: Notification Letter Medtronic HVAD™ System|url=https://www.medtronic.com/content/dam/medtronic-com/global/HCP/Documents/hvad-urgent-medical-device-notice-june-2021.pdf|access-date=September 30, 2021}}</ref> |
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The majority of VADs on the market today are somewhat bulky. The smallest device approved by the FDA, the HeartMate II, weighs about {{convert|1|lb|kg}} and measures {{convert|3|in|cm}}. This has proven particularly important for women and children, for whom alternatives would have been too large.<ref>{{cite journal |author= Bogaev, R |author2=Chen, L |author3=Russell, SD|display-authors=etal |year= 2007 |title=Medical Aspects of End-Stage Heart Failure: Transplantation and Device Therapies I, Abstract 1762: An Emerging Option for Women with Advanced Heart Failure: Results of the HeartMate II Continuous Flow Left Ventricular Assist Device Bridge to Transplant Trial|journal= [[Circulation (journal)|Circulation]] |volume= 116 |page= 372 |publisher= American Heart Association|url= http://circ.ahajournals.org/cgi/content/meeting_abstract/116/16_MeetingAbstracts/II_372-c|archive-url=https://web.archive.org/web/20110608220036/http://circ.ahajournals.org/cgi/content/meeting_abstract/116/16_MeetingAbstracts/II_372-c|archive-date=8 June 2011}}</ref> As of 2017, HeartMate III has been approved by the FDA. It is smaller than its predecessor HeartMate II and uses a full maglev impeller instead of the cup-and-ball bearing system found in HeartMate II.<ref>{{Cite web |url=https://www.thoratec.com/medical-professionals/vad-product-information/heartmate3/HeartMate3_PressKit-UK.pdf |title=Archived copy |access-date=9 January 2018 |archive-date=10 January 2018 |archive-url=https://web.archive.org/web/20180110054816/https://www.thoratec.com/medical-professionals/vad-product-information/heartmate3/HeartMate3_PressKit-UK.pdf |url-status=dead }}</ref> |
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The HeartWare HVAD works similarly to the VentrAssist—albeit much smaller and not requiring an abdominal pocket to be implanted into. The device has obtained CE Mark in Europe, and FDA approval in the U.S. The HeartWare HVAD could be implanted through limited access without [[sternotomy]], however in 2021 Medtronic discontinued the device.<ref>{{Cite journal | last1 = Popov | first1 = AF | last2 = Hosseini | first2 = MT | last3 = Zych | first3 = B|display-authors=etal| title = HeartWare Left Ventricular Assist Device Implantation Through Bilateral Anterior Thoracotomy | doi = 10.1016/j.athoracsur.2011.09.055 | journal = [[The Annals of Thoracic Surgery]] | volume = 93 | issue = 2 | pages = 674–676 | year = 2012 | pmid = 22269746 }}</ref><ref name=":1" /> |
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* [[HeartWare International]] announced in August 2009 that it had surpassed 50 implants of their HeartWare Ventricular Assist System in their ADVANCE Clinical Trial, an FDA-approved IDE study. The study is to assess the system as bridge-to-transplantation for patients with end-stage heart failure. The study, Evaluation of the HeartWare LVAD System for the Treatment of Advanced Heart Failure, is a multi-center study that started in May 2009.<ref>{{cite news |title= Evaluation of the HeartWare LVAD System for the Treatment of Advanced Heart Failure |url= http://www.hopkinsmedicine.org/heart_vascular_institute/clinical_trials/mechanical_circulatory_support/heartware_lvad_system_heart_failure.html|publisher= [[Johns Hopkins Medical Center]] |date= May 2009}}</ref><ref>{{cite news |title= HeartWare International Surpasses 50 Implants in the US |url= http://www.bio-medicine.org/medicine-news-1/HeartWare-International-Surpasses-50-Implants-in-the-US-54995-1/|newspaper= Bio-Medicine |date= 20 August 2009}}</ref> |
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*On June 27, 2014 Hannover Medical School in Hannover, Germany performed the first human implant of HeartMate III under the direction of professor Axel Haverich M.D., chief of the Cardiothoracic, Transplantation and Vascular Surgery Department and surgeon Jan Schmitto, M.D., Ph.D.<ref>{{cite news|title= Thoratec Announces First HeartMate III Human Implant And Start Of CE Mark Trial|url= http://phx.corporate-ir.net/phoenix.zhtml?c=95989&p=irol-newsArticle&ID=1943285|archive-url= https://archive.is/20141007133132/http://phx.corporate-ir.net/phoenix.zhtml?c=95989&p=irol-newsArticle&ID=1943285|url-status= dead|archive-date= 7 October 2014|publisher= Thoratec Corporation|date= 20 August 2009}}</ref> |
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*On January 21, 2015 a study was published in Journal of American College of Cardiology suggesting that long-term use of LVAD may induce heart regeneration.<ref>{{cite journal | year = 2015 | title = Human Ventricular Unloading Induces Cardiomyocyte Proliferation| url = | journal = [[Journal of the American College of Cardiology]] | volume = 65 | issue = 9| pages = 892–900 | doi = 10.1016/j.jacc.2014.12.027 | pmc = 4488905| last1 = Canseco| first1 = Diana C.| last2 = Kimura| first2 = Wataru| last3 = Garg| first3 = Sonia| last4 = Mukherjee| first4 = Shibani| last5 = Bhattacharya| first5 = Souparno| last6 = Abdisalaam| first6 = Salim| last7 = Das| first7 = Sandeep| last8 = Asaithamby| first8 = Aroumougame| last9 = Mammen| first9 = Pradeep P.A.| last10 = Sadek| first10 = Hesham A. | pmid=25618530}}</ref> This may explain the bridge to recovery phenomenon first described by the Yacoub group in NEJM in 2009 (above).{{citation needed|date=July 2016}} |
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*Hall-of-Fame Baseball Player Rod Carew had congestive heart failure and was fitted with a HeartMate II. He struggled with wearing the equipment, so he joined efforts to help supply the most helpful wear to assist the HeartMate II and HeartMate III.<ref>{{Cite web|url=http://www.carewmedicalwear.com|title=LVAD Wear|last=|first=|date=|website=www.carewmedicalwear.com|language=en-US}}</ref> |
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The majority of VADs on the market today are somewhat bulky. The smallest device approved by the FDA, the HeartMate II, weighs about {{convert|1|lb|kg}} and measures {{convert|3|in|cm}}. This has proven particularly important for women and children, for whom alternatives would have been too large.<ref>{{cite journal |author= Bogaev, R |author2=Chen, L |author3=Russell, SD|display-authors=etal |year= 2007 |title=Medical Aspects of End-Stage Heart Failure: Transplantation and Device Therapies I, Abstract 1762: An Emerging Option for Women with Advanced Heart Failure: Results of the HeartMate II Continuous Flow Left Ventricular Assist Device Bridge to Transplant Trial|journal= [[Circulation (journal)|Circulation]] |volume= 116 |series= II |page= 372 |publisher= American Heart Association|url= http://circ.ahajournals.org/cgi/content/meeting_abstract/116/16_MeetingAbstracts/II_372-c|archiveurl=https://web.archive.org/web/20110608220036/http://circ.ahajournals.org/cgi/content/meeting_abstract/116/16_MeetingAbstracts/II_372-c|archivedate=8 June 2011}}</ref> As of 2017, HeartMate III has been approved by the FDA. It is smaller than its predecessor HeartMate II, and uses a full maglev impeller instead of the cup-and-ball bearing system found in HeartMate II.<ref>https://www.thoratec.com/medical-professionals/vad-product-information/heartmate3/HeartMate3_PressKit-UK.pdf</ref> |
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One device, VentrAssist, gained CE Mark approval for use in the EU and began clinical trials in the US. As of June 2007 these pumps had been implanted in over 100 patients. In 2009, Ventracor was placed into the hands of Administrators due to financial problems and was later that year liquidated. No other companies purchased the technology, so as a result the VentrAssist device was essentially defunct. Around 30–50 patients worldwide remain supported on VentrAssist devices as of January 2010.{{Citation needed|date=June 2013}} |
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The HeartWare HVAD works similarly to the VentrAssist—albeit much smaller and not requiring an abdominal pocket to be implanted into. The device has obtained CE Mark in Europe, and FDA approval in the U.S. Recently, it was shown that the HeartWare HVAD can be implanted through limited access without [[sternotomy]].<ref>{{Cite journal | last1 = Popov | first1 = AF | last2 = Hosseini | first2 = MT | last3 = Zych | first3 = B|display-authors=etal| title = HeartWare Left Ventricular Assist Device Implantation Through Bilateral Anterior Thoracotomy | doi = 10.1016/j.athoracsur.2011.09.055 | journal = [[The Annals of Thoracic Surgery]] | volume = 93 | issue = 2 | pages = 674–676 | year = 2012 | pmid = 22269746 }}</ref> |
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In a small number of cases left ventricular assist devices, combined with drug therapy, have enabled the heart to recover sufficiently for the device to be able to be removed (''explanted'').<ref name="content.nejm.org"/><ref name="ventracor.com"/> Several surgical approaches, including interventional decommissioning, off-pump explantation using a custom-made plug and complete LVAD removal through redo sternotomy, have been described with a 5-year survival of up to 80%.<ref>{{cite journal |last1=Potapov |first1=EV |last2=Politis |first2=N |last3=Karck |first3=M |last4=Weyand |first4=M |last5=Tandler |first5=R |last6=Walther |first6=T |last7=Emrich |first7=F |last8=Reichenspurrner |first8=H |last9=Bernhardt |first9=A |last10=Barten |first10=MJ |last11=Svenarud |first11=P |last12=Gummert |first12=J |last13=Sef |first13=D |last14=Doenst |first14=T |last15=Tsyganenko |first15=D |last16=Loforte |first16=A |last17=Schoenrath |first17=F |last18=Falk |first18=V |title=Results from a multicentre evaluation of plug use for left ventricular assist device explantation. |journal=Interactive Cardiovascular and Thoracic Surgery |date=31 March 2022 |volume=34 |issue=4 |pages=683–690 |doi=10.1093/icvts/ivab344 |pmid=34888681|pmc=9026212 }}</ref> |
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In a small number of cases left ventricular assist devices, combined with drug therapy, have enabled the heart to recover sufficiently for the device to be able to be removed (''explanted'').<ref name="content.nejm.org"/><ref name="ventracor.com"/> |
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===HeartMate II LVAD pivotal study=== |
===HeartMate II LVAD pivotal study=== |
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A series of studies involving the use of the HeartMate II LVAD have proven useful in establishing the viability and risks of using LVADs for bridge-to-transplantation and destination therapy. |
A series of studies involving the use of the HeartMate II LVAD have proven useful in establishing the viability and risks of using LVADs for bridge-to-transplantation and destination therapy. |
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* The HeartMate II [[pivotal trial]] began in 2005 and included the evaluation of HeartMate II for two indications: Bridge to transplantation (BTT) and destination therapy (DT), or long-term, permanent support. Thoratec Corp. announced that this was the first time the FDA had approved a clinical trial to include both indications in one protocol.<ref name=thor_hm2_piv>{{cite news |first= Susan |last= Benton |title= HeartMate II Pivotal Clinical Trial Fact Sheet|url= http://www.thoratec.com/downloads/heartmate-ii-pivotal-clinical-trial-fact-sheet-081909.pdf |publisher= Thoratec Corporation |date= 19 August 2008 |access-date=10 September 2009 }}</ref><ref name=crsti_hm2_piv>{{cite news |first= Todd |last= Dewey |title= The HeartMate II LVAS Pivotal Trial |url= http://www.crsti.org/protocols/heartmate-2.html |publisher= Cardiopulmonary Research Science and Technology Institute |date= 19 August 2008 |archive-url = https://web.archive.org/web/20070713184120/http://www.crsti.org/protocols/heartmate-2.html |archive-date = 13 July 2007 }}</ref><ref name=nypresb_hm2>{{cite news |first= Belinda |last= Mager |title= FDA Approves HeartMate II Mechanical Heart Pump for Heart-Failure Patients Waiting for Organ Transplantation |url= http://nyp.org/news/hospital/heartmateII-organ-transplantation.html |archive-date=8 May 2008|archive-url=https://web.archive.org/web/20080508074333/http://www.nyp.org/news/hospital/heartmateII-organ-transplantation.html|publisher= [[NewYork–Presbyterian Hospital]] |date= 25 April 2008}}</ref> |
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* A multicenter study in the United States from 2005 to 2007 with 113 patients (of which 100 reported principal outcomes) showed that significant improvements in function were prevalent after three months, and a survival rate of 68% after twelve months.<ref name=njem_aug07>{{Cite journal | last1 = Miller | first1 = LW | last2 = Pagani | first2 = FD | last3 = Russell | first3 = SD|display-authors=etal | doi = 10.1056/NEJMoa067758 | title = Use of a Continuous-Flow Device in Patients Awaiting Heart Transplantation | journal = [[New England Journal of Medicine]] | volume = 357 | issue = 9 | pages = 885–896 | year = 2007 | pmid = 17761592 | doi-access = free }}</ref> |
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* The pilot trial for the HeartMate II LVAD began in November 2003 and consisted of 46 study patients at 15 centers. Results included 11 patients supported for more than one year and three patients supported for more than two years. |
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* Based on one-year follow up data from the first 194 patients enrolled in the trial, the FDA approved HeartMate II for bridge-to-transplantation. The trial provided clinical evidence of improved survival rates and quality of life for a broad range of patients.<ref name=umhs>{{cite news |first= Kara |last= Gavin |title=Exciting times for heart-assisting devices at U-M |url=http://www2.med.umich.edu/prmc/media/newsroom/details.cfm?ID=179 |publisher= University of Michigan Health System |date= 23 April 2008|archive-url=https://web.archive.org/web/20080510224935/http://www2.med.umich.edu/prmc/media/newsroom/details.cfm?ID=179|archive-date=10 May 2008}}</ref><ref name=fda_heartmate_ii>{{cite news |title=Thoratec HeartMate II LVAS – P060040 | url=https://www.fda.gov/MedicalDevices/ProductsandMedicalProcedures/DeviceApprovalsandClearances/Recently-ApprovedDevices/ucm074231.htm |agency= [[Food and Drug Administration]] |date= 23 April 2008 |access-date=28 August 2009 }}</ref> |
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* The HeartMate II [[pivotal trial]] began in 2005 and included the evaluation of HeartMate II for two indications: Bridge to transplantation (BTT) and destination therapy (DT), or long-term, permanent support. Thoratec Corp. announced that this was the first time the FDA had approved a clinical trial to include both indications in one protocol.<ref name=thor_hm2_piv>{{cite news |first= Susan |last= Benton |title= HeartMate II Pivotal Clinical Trial Fact Sheet|url= http://www.thoratec.com/downloads/heartmate-ii-pivotal-clinical-trial-fact-sheet-081909.pdf |publisher= Thoratec Corporation |date= 19 August 2008 |accessdate=10 September 2009 }}</ref><ref name=crsti_hm2_piv>{{cite news |first= Todd |last= Dewey |title= The HeartMate II LVAS Pivotal Trial |url= http://www.crsti.org/protocols/heartmate-2.html |publisher= Cardiopulmonary Research Science and Technology Institute |date= 19 August 2008 |archiveurl = https://web.archive.org/web/20070713184120/http://www.crsti.org/protocols/heartmate-2.html |archivedate = 13 July 2007 }}</ref><ref name=nypresb_hm2>{{cite news |first= Belinda |last= Mager |title= FDA Approves HeartMate II Mechanical Heart Pump for Heart-Failure Patients Waiting for Organ Transplantation |url= http://nyp.org/news/hospital/heartmateII-organ-transplantation.html |archivedate=8 May 2008|archiveurl=https://web.archive.org/web/20080508074333/http://www.nyp.org/news/hospital/heartmateII-organ-transplantation.html|publisher= [[NewYork–Presbyterian Hospital]] |date= 25 April 2008}}</ref> |
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* Eighteen-month follow up data on 281 patients who had either reached the study end-point or completed 18 months of post-operative follow-up showed improved survival, less frequent adverse events and greater reliability with continuous flow LVADS compared to pulsatile flow devices. Of the 281 patients, 157 patients had undergone transplant, 58 patients were continuing with LVADs in their body and seven patients had the LVAD removed because their heart recovered; the remaining 56 had died. The results showed that the patients' [[New York Heart Association Functional Classification|NYHA Class]] of heart failure had significantly improved after six months of LVAD support compared to the pre-LVAD baseline. Although this trial involved bridge-to-transplant indication, the results provide early evidence that continuous flow LVADs have advantages in terms of durability and reliability for patients receiving mechanical support for destination therapy.<ref>{{Cite journal | last1 = Eisen | first1 = HJ | last2 = Hankins | first2 = SR | doi = 10.1016/j.jacc.2009.04.028 | title = Continuous Flow Rotary Left Ventricular Assist Device | journal = [[Journal of the American College of Cardiology]] | volume = 54 | issue = 4 | pages = 322–324 | year = 2009 | pmid = 19608029 | doi-access = free }}</ref> |
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* A multicenter study in the United States from 2005 to 2007 with 113 patients (of which 100 reported principal outcomes) showed that significant improvements in function were prevalent after three months, and a survival rate of 68% after twelve months.<ref name=njem_aug07>{{Cite journal | last1 = Miller | first1 = LW | last2 = Pagani | first2 = FD | last3 = Russell | first3 = SD|display-authors=etal | doi = 10.1056/NEJMoa067758 | title = Use of a Continuous-Flow Device in Patients Awaiting Heart Transplantation | journal = [[New England Journal of Medicine]] | volume = 357 | issue = 9 | pages = 885–896 | year = 2007 | pmid = 17761592 }}</ref> |
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* Based on one-year follow up data from the first 194 patients enrolled in the trial, the FDA approved HeartMate II for bridge-to-transplantation. The trial provided clinical evidence of improved survival rates and quality of life for a broad range of patients.<ref name=umhs>{{cite news |first= Kara |last= Gavin |title=Exciting times for heart-assisting devices at U-M |url=http://www2.med.umich.edu/prmc/media/newsroom/details.cfm?ID=179 |publisher= University of Michigan Health System |date= 23 April 2008|archiveurl=https://web.archive.org/web/20080510224935/http://www2.med.umich.edu/prmc/media/newsroom/details.cfm?ID=179|archivedate=10 May 2008}}</ref><ref name=fda_heartmate_ii>{{cite news |title=Thoratec HeartMate II LVAS – P060040 | url=https://www.fda.gov/MedicalDevices/ProductsandMedicalProcedures/DeviceApprovalsandClearances/Recently-ApprovedDevices/ucm074231.htm |agency= [[Food and Drug Administration]] |date= 23 April 2008 |accessdate=28 August 2009 }}</ref> |
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* Eighteen-month follow up data on 281 patients who had either reached the study end-point or completed 18 months of post-operative follow-up showed improved survival, less frequent adverse events and greater reliability with continuous flow LVADS compared to pulsatile flow devices. Of the 281 patients, 157 patients had undergone transplant, 58 patients were continuing with LVADs in their body and seven patients had the LVAD removed because their heart recovered; the remaining 56 had died. The results showed that the NYHA Class of heart failure the patients had been designated had significantly improved after six months of LVAD support compared to the pre-LVAD baseline. Although this trial involved bridge-to-transplant indication, the results provide early evidence that continuous flow LVADs have advantages in terms of durability and reliability for patients receiving mechanical support for destination therapy.<ref>{{Cite journal | last1 = Eisen | first1 = HJ | last2 = Hankins | first2 = SR | doi = 10.1016/j.jacc.2009.04.028 | title = Continuous Flow Rotary Left Ventricular Assist Device | journal = [[Journal of the American College of Cardiology]] | volume = 54 | issue = 4 | pages = 322–324 | year = 2009 | pmid = 19608029 }}</ref> |
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* Following the FDA approval of HeartMate II LVAD for bridge-to-transplantation purposes, a post-approval ("registry") study was undertaken to assess the efficacy of the device in a commercial setting. The study found that the device improved outcomes, both compared to other LVAD treatments and baseline patients. Specifically, HeartMate II patients showed lower creatinine levels, 30-day survival rates were considerably higher at 96%, and 93% reached successful outcomes (transplant, cardiac recovery, or long-term LVAD).<ref name=JoCFAug09>{{cite journal |author= Starling, RC |author2=Naka, Y |author3=Boyle, AJ|display-authors=etal |date=Aug 2009 |title= Initial FDA Post-Approval Study INTERMACS Registry Results with a Continuous Flow Left Ventricular Assist Device as a Bridge to Heart Transplantation |journal= Journal of Cardiac Failure |volume= 15 |issue= 6 |page= S46 |doi= 10.1016/j.cardfail.2009.06.252}}</ref> |
* Following the FDA approval of HeartMate II LVAD for bridge-to-transplantation purposes, a post-approval ("registry") study was undertaken to assess the efficacy of the device in a commercial setting. The study found that the device improved outcomes, both compared to other LVAD treatments and baseline patients. Specifically, HeartMate II patients showed lower creatinine levels, 30-day survival rates were considerably higher at 96%, and 93% reached successful outcomes (transplant, cardiac recovery, or long-term LVAD).<ref name=JoCFAug09>{{cite journal |author= Starling, RC |author2=Naka, Y |author3=Boyle, AJ|display-authors=etal |date=Aug 2009 |title= Initial FDA Post-Approval Study INTERMACS Registry Results with a Continuous Flow Left Ventricular Assist Device as a Bridge to Heart Transplantation |journal= Journal of Cardiac Failure |volume= 15 |issue= 6 |page= S46 |doi= 10.1016/j.cardfail.2009.06.252}}</ref> |
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===HARPS=== |
===HARPS=== |
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The Harefield Recovery Protocol Study (HARPS) is a clinical trial to evaluate whether advanced heart failure patients requiring VAD support can recover sufficient myocardial function to allow device removal (known as explantation). HARPS combines an LVAD (the HeartMate XVE) with conventional oral heart failure medications, followed by the novel β2 agonist clenbuterol. This opens the possibility that some advanced heart failure patients may forgo heart transplantation.<ref name=HARPS_01>{{cite journal |last=Miller |first=Leslie |author2=Aaronson and Pagani |year= 2008 |title= Harefield Recovery Protocol Study for Patients With Refractory Chronic Heart Failure (HARPS) |journal= ClinicalTrials.gov |url= http://clinicaltrials.gov/ct2/show/NCT00585546 | |
The Harefield Recovery Protocol Study (HARPS) is a clinical trial to evaluate whether advanced heart failure patients requiring VAD support can recover sufficient myocardial function to allow device removal (known as explantation). HARPS combines an LVAD (the HeartMate XVE) with conventional oral heart failure medications, followed by the novel β2 agonist [[clenbuterol]]. This opens the possibility that some advanced heart failure patients may forgo heart transplantation.<ref name=HARPS_01>{{cite journal |last=Miller |first=Leslie |author2=Aaronson and Pagani |year= 2008 |title= Harefield Recovery Protocol Study for Patients With Refractory Chronic Heart Failure (HARPS) |journal= ClinicalTrials.gov |url= http://clinicaltrials.gov/ct2/show/NCT00585546 |access-date= 2009-08-03}}</ref> |
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To date, 73% (11 of 15) of patients who underwent the combination therapy regimen demonstrated sufficient recovery to allow explantation and avoid heart transplantation; freedom from recurrent heart failure in surviving patients was 100% and 89% at one and four years after explantation, respectively; average ejection fraction was 64% at 59 months after explantation—all patients were NYHA Class I; and no significant adverse effects were reported with clenbuterol therapy. |
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===REMATCH=== |
===REMATCH=== |
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The REMATCH (Randomized Evaluation of Mechanical Assistance for the Treatment of Congestive Heart Failure) clinical trial began in May 1998 and ran through July 2001 in 20 cardiac transplant centers around the USA. The trial was designed to compare long-term implantation of left ventricular assist devices with optimal medical management for patients with end-stage heart failure who require, but do not qualify to receive cardiac transplantation. As a result of the clinical outcomes, the device received FDA approval for both indications, in 2001 and 2003, respectively.<ref name=rematch_ats>{{Cite journal | doi = 10.1016/S0003-4975(99)00042-9 | last1 = Rose | first1 = EA | last2 = Moskowitz | first2 = AJ | last3 = Packer | first3 = M|display-authors=etal | title = The REMATCH trial: Rationale, design, and end points. Randomized Evaluation of Mechanical Assistance for the Treatment of Congestive Heart Failure | journal = [[The Annals of Thoracic Surgery]] | volume = 67 | issue = 3 | pages = 723–730 | year = 1999 | pmid = 10215217 }}</ref> |
The REMATCH (Randomized Evaluation of Mechanical Assistance for the Treatment of Congestive Heart Failure) clinical trial began in May 1998 and ran through July 2001 in 20 cardiac transplant centers around the USA. The trial was designed to compare long-term implantation of left ventricular assist devices with optimal medical management for patients with end-stage heart failure who require, but do not qualify to receive cardiac transplantation. As a result of the clinical outcomes, the device received FDA approval for both indications, in 2001 and 2003, respectively.<ref name=rematch_ats>{{Cite journal | doi = 10.1016/S0003-4975(99)00042-9 | last1 = Rose | first1 = EA | last2 = Moskowitz | first2 = AJ | last3 = Packer | first3 = M|display-authors=etal | title = The REMATCH trial: Rationale, design, and end points. Randomized Evaluation of Mechanical Assistance for the Treatment of Congestive Heart Failure | journal = [[The Annals of Thoracic Surgery]] | volume = 67 | issue = 3 | pages = 723–730 | year = 1999 | pmid = 10215217 | doi-access = free }}</ref> |
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According to a retrospective cohort study comparing patients treated with a left ventricular assist device versus inotrope therapy while awaiting heart transplantation, the group treated with LVAD had improved clinical and metabolic function at the time of transplant with better blood pressure, sodium, blood urea nitrogen, and creatinine. After transplant, 57.7% of the inotrope group had [[kidney failure]] versus 16.6% in the LVAD group; 31.6% of the inotrope group had right heart failure versus 5.6% in the LVAD group; and event-free survival was 15.8% in the inotrope group versus 55.6% in the LVAD group.<ref name=intrepid>{{Cite journal | last1 = Rogers | first1 = JG | last2 = Butler | first2 = J | last3 = Lansman | first3 = SL|display-authors=etal | title = Chronic Mechanical Circulatory Support for Inotrope-Dependent Heart Failure Patients Who Are Not Transplant Candidates | doi = 10.1016/j.jacc.2007.03.063 | journal = [[Journal of the American College of Cardiology]] | volume = 50 | issue = 8 | pages = 741–747 | year = 2007 | pmid = 17707178 | doi-access = }}</ref> |
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The trial demonstrated an 81% improvement in two-year survival among patients receiving HeartMate XVE compared to optimal medical management. In addition, a destination therapy study following the REMATCH trial demonstrated an additional 17% improvement (61% vs. 52%) in one-year survival of patients that were implanted with a VAD (HeartMate XVE), with an implication for the appropriate selection of candidates and timing of VAD implantation. |
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==Complications and side effects== |
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A test carried out in 2001 by [[Eric Rose|Dr. Eric A. Rose]] and REMATCH study group with patients with congestive heart failure that were ineligible for a transplant showed a survival at two years of 23% for those implanted with an LVAD compared with 8% for those who were treated with drugs. The two major complications of VAD implantation were infection and mechanical failure (see below). |
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There are a number of potential risks associated with VADs. The most common of these are bleeding events, stroke, pump thrombosis, and infections.<ref name="Varshney 1092–1107">{{Cite journal |last1=Varshney |first1=Anubodh S. |last2=DeFilippis |first2=Ersilia M. |last3=Cowger |first3=Jennifer A. |last4=Netuka |first4=Ivan |last5=Pinney |first5=Sean P. |last6=Givertz |first6=Michael M. |date=2022-03-22 |title=Trends and Outcomes of Left Ventricular Assist Device Therapy: JACC Focus Seminar |journal=Journal of the American College of Cardiology |volume=79 |issue=11 |pages=1092–1107 |doi=10.1016/j.jacc.2022.01.017 |issn=1558-3597 |pmid=35300822|doi-access=free }}</ref> |
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According to a retrospective cohort study comparing patients treated with a left ventricular assist device versus inotrope therapy while awaiting heart transplantation, the group treated with LVAD had improved clinical and metabolic function at the time of transplant with better blood pressure, sodium, blood urea nitrogen, and creatinine. After transplant, 57.7% of the inotrope group had [[kidney failure]] versus 16.6% in the LVAD group; 31.6% of the inotrope group had right heart failure versus 5.6% in the LVAD group; and event-free survival was 15.8% in the inotrope group versus 55.6% in the LVAD group.<ref name=intrepid>{{Cite journal | last1 = Rogers | first1 = JG | last2 = Butler | first2 = J | last3 = Lansman | first3 = SL|display-authors=etal | title = Chronic Mechanical Circulatory Support for Inotrope-Dependent Heart Failure Patients Who Are Not Transplant Candidates | doi = 10.1016/j.jacc.2007.03.063 | journal = [[Journal of the American College of Cardiology]] | volume = 50 | issue = 8 | pages = 741–747 | year = 2007 | pmid = 17707178 }}</ref> |
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'''Bleeding''' |
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==Complications and side effects== |
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Bleeding is the most common postoperative early complication after implantation or explantation of LVADs, necessitating reoperation in up to 60% of recipients.<ref name=Schaffer>{{cite journal|last=Schaffer|first=JM|author2=Arnaoutakis, GJ |author3=Allen, JG|display-authors=etal|title=Bleeding Complications and Blood Product Utilization With Left Ventricular Assist Device Implantation|journal=[[The Annals of Thoracic Surgery]]|volume=91|issue=3|pages=740–749|doi=10.1016/j.athoracsur.2010.11.007|year=2011}}</ref><ref name=Goldstein>{{cite journal|last=Goldstein|first=Daniel J.|author2=Robert B. Beauford |title=Left ventricular assist devices and bleeding: adding insult to injury|journal=[[The Annals of Thoracic Surgery]]|year=2003|volume=75|issue=6|pages=S42–7|pmid=12820734|doi=10.1016/s0003-4975(03)00478-8}}</ref> The implications of massive blood transfusions are great and include infection, pulmonary insufficiency, increased costs, right heart failure, allosensitization, and viral transmission, some of which can prove fatal or preclude transplantation.<ref name=Goldstein /> When bleeding occurs, it impacts the one year Kaplan-Meier mortality.<ref name=Schaffer /> In addition to complexity of the patient population and the complexity of these procedures contributing to bleeding, the devices themselves may contribute to the severe coagulopathy that can ensue when these devices are implanted.<ref name=Spanier>{{cite journal|last=Spanier|first=Talia|author2=Oz, M |author3=Levin, H|display-authors=etal |title=Activation of coagulation and fibrinolytic pathways with left ventricular assist devices|journal=Journal of Thoracic and Cardiovascular Surgery|year=1996|volume=112|pages=1090–1097|pmid=8873737|doi=10.1016/s0022-5223(96)70111-3}}</ref> |
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Because the VADs generally result in blood flowing over a non-biologic surface (e.g. metal, synthetic polymers, etc.) this can result in formation of blood clots, also referred to as [[thrombosis]]. Due to these [[Coagulation|clotting]] abnormalities, [[anticoagulation]] medications are used to decrease the risk of thrombosis. One device, the HeartMate XVE, is designed with a biologic surface derived from [[fibrin]] and does not require long term anticoagulation (except aspirin); unfortunately, this biologic surface may also predispose the patient to infection through selective reduction of certain types of leukocytes, however this device was phased out of use starting in 2009 in favor of newer devices.<ref>{{Cite journal |last1=Stansfield |first1=William E. |last2=Rao |first2=Vivek |date=September 2016 |title=HeartMate 3: Facing the challenge of past success |journal=The Journal of Thoracic and Cardiovascular Surgery |volume=152 |issue=3 |pages=683–685 |doi=10.1016/j.jtcvs.2016.04.048 |issn=1097-685X |pmid=27210469|doi-access=free }}</ref><ref name="ats_anticoag">{{Cite journal |last1=Samuels |first1=LE |last2=Kohout |first2=J |last3=Casanova-Ghosh |first3=E |display-authors=etal |year=2008 |title=Argatroban as a Primary or Secondary Postoperative Anticoagulant in Patients Implanted with Ventricular Assist Devices |journal=[[The Annals of Thoracic Surgery]] |volume=85 |issue=5 |pages=1651–1655 |doi=10.1016/j.athoracsur.2008.01.100 |pmid=18442558}}</ref> |
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Due to the use of anticoagulation, bleeding is the most common postoperative early complication after implantation or explantation of VADs, necessitating reoperation in up to 60% of recipients.<ref name="Schaffer">{{cite journal|last=Schaffer|first=JM|author2=Arnaoutakis, GJ |author3=Allen, JG|display-authors=etal|title=Bleeding Complications and Blood Product Utilization With Left Ventricular Assist Device Implantation|journal=[[The Annals of Thoracic Surgery]]|volume=91|issue=3|pages=740–749|doi=10.1016/j.athoracsur.2010.11.007|year=2011|pmid=21352991|doi-access=free}}</ref><ref name="Goldstein">{{cite journal|last=Goldstein|first=Daniel J.|author2=Robert B. Beauford |title=Left ventricular assist devices and bleeding: adding insult to injury|journal=[[The Annals of Thoracic Surgery]]|year=2003|volume=75|issue=6|pages=S42–7|pmid=12820734|doi=10.1016/s0003-4975(03)00478-8}}</ref> Most commonly bleeding occurs in the gastrointestinal tract resulting in dark or bright red stools,<ref>{{Cite journal |last1=Naveed |first1=Ali |last2=Naveed |first2=Bazigh |last3=Khan |first3=Muhammad Atif |last4=Asif |first4=Talal |date=September 2023 |title=Gastrointestinal bleeding in recipients of left ventricular assist devices-a systematic review |url=https://pubmed.ncbi.nlm.nih.gov/37145271 |journal=Heart Failure Reviews |volume=28 |issue=5 |pages=1163–1175 |doi=10.1007/s10741-023-10313-6 |issn=1573-7322 |pmid=37145271}}</ref> however if trauma to the head occurs, intracranial bleeding may also occur.<ref>{{Cite journal |last1=Elder |first1=Theresa |last2=Raghavan |first2=Alankrita |last3=Smith |first3=Arvin |last4=Wright |first4=Christina Huang |last5=Wright |first5=James |last6=Burant |first6=Christopher |last7=Sajatovic |first7=Martha |last8=Hoffer |first8=Alan |date=December 2019 |title=Outcomes After Intracranial Hemorrhage in Patients with Left Ventricular Assist Devices: A Systematic Review of Literature |url=https://pubmed.ncbi.nlm.nih.gov/31493616 |journal=World Neurosurgery |volume=132 |pages=265–272 |doi=10.1016/j.wneu.2019.08.211 |issn=1878-8769 |pmid=31493616}}</ref> Bleeding events may require massive blood transfusions and incur certain risks including infection, pulmonary insufficiency, increased costs, right heart failure, allosensitization, and viral transmission, which can prove fatal or preclude transplantation.<ref name="Goldstein" /> When bleeding occurs, it impacts the one year Kaplan-Meier mortality.<ref name="Schaffer" /> In addition to complexity of the patient population and the complexity of these procedures contributing to bleeding, the devices themselves may contribute to the severe coagulopathy that can ensue when these devices are implanted.<ref name="Spanier">{{cite journal|last=Spanier|first=Talia|author2=Oz, M |author3=Levin, H|display-authors=etal |title=Activation of coagulation and fibrinolytic pathways with left ventricular assist devices|journal=Journal of Thoracic and Cardiovascular Surgery|year=1996|volume=112|issue=4|pages=1090–1097|pmid=8873737|doi=10.1016/s0022-5223(96)70111-3|doi-access=free}}</ref> |
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'''Ischemic Stroke and Pump Thrombosis''' |
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In patients with VADs, ischemic strokes and pump thrombosis occur when there is inadequate anticoagulation to counter act the blood's tendency to form blood clots when exposed to the foreign materials in a VAD. Stroke risk varies based on the type of VAD in place and other risk factors.<ref name="Varshney 1092–1107"/> Both atrial fibriliation and high blood pressure may increase risk of stroke and high blood pressure can increase a patient's risk of stroke in the setting of VAD use.<ref>{{Cite journal |last1=Varshney |first1=Anubodh S. |last2=DeFilippis |first2=Ersilia M. |last3=Cowger |first3=Jennifer A. |last4=Netuka |first4=Ivan |last5=Pinney |first5=Sean P. |last6=Givertz |first6=Michael M. |date=2022-03-22 |title=Trends and Outcomes of Left Ventricular Assist Device Therapy: JACC Focus Seminar |journal=Journal of the American College of Cardiology |volume=79 |issue=11 |pages=1092–1107 |doi=10.1016/j.jacc.2022.01.017 |issn=0735-1097|doi-access=free |pmid=35300822 }}</ref> However, it is difficult to measure blood pressure in LVAD patients using standard blood pressure monitoring and the current practice is to measure by [[Doppler ultrasonography]] in [[outpatients]] and invasive [[arterial blood pressure]] monitoring in [[inpatients]].<ref>{{Cite journal|last1=Castagna|first1=Francesco|last2=Stöhr|first2=Eric J.|last3=Pinsino|first3=Alberto|last4=Cockcroft|first4=John R.|last5=Willey|first5=Joshua|last6=Reshad Garan|first6=A.|last7=Topkara|first7=Veli K.|last8=Colombo|first8=Paolo C.|last9=Yuzefpolskaya|first9=Melana|last10=McDonnell|first10=Barry J.|date=2017|title=The Unique Blood Pressures and Pulsatility of LVAD Patients: Current Challenges and Future Opportunities|journal=Current Hypertension Reports|volume=19|issue=10|page=85|doi=10.1007/s11906-017-0782-6|issn=1522-6417|pmc=5645430|pmid=29043581}}</ref> |
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Because the devices generally result in blood flowing over a non-biologic surface, predisposing the blood to [[Coagulation|clotting]], there is need for [[anticoagulation]] measures. One device, the HeartMate XVE, is designed with a biologic surface derived from [[fibrin]] and does not require long term anticoagulation (except aspirin); unfortunately, this biologic surface may also predispose the patient to infection through selective reduction of certain types of leukocytes.<ref name=ats_anticoag>{{Cite journal | last1 = Samuels | first1 = LE | last2 = Kohout | first2 = J | last3 = Casanova-Ghosh | first3 = E|display-authors=etal | doi = 10.1016/j.athoracsur.2008.01.100 | title = Argatroban as a Primary or Secondary Postoperative Anticoagulant in Patients Implanted with Ventricular Assist Devices | journal = [[The Annals of Thoracic Surgery]] | volume = 85 | issue = 5 | pages = 1651–1655 | year = 2008 | pmid = 18442558 }}</ref> |
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'''Infections''' |
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New VAD designs which are now approved for use in the European Community and are undergoing trials for FDA approval have all but eliminated mechanical failure.{{Citation needed|date=June 2013}} |
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Infections in VAD patients occur because the artificial surfaces of the devices serve as a surface for bacterial and or fungal growth.<ref name="O'Horo 2018 287–294">{{Cite journal |last1=O'Horo |first1=John C. |last2=Abu Saleh |first2=Omar M. |last3=Stulak |first3=John M. |last4=Wilhelm |first4=Mark P. |last5=Baddour |first5=Larry M. |last6=Rizwan Sohail |first6=M. |date=2018 |title=Left Ventricular Assist Device Infections: A Systematic Review |journal=ASAIO Journal |volume=64 |issue=3 |pages=287–294 |doi=10.1097/MAT.0000000000000684 |issn=1538-943X |pmc=5920737 |pmid=29095732}}</ref> Most infections are classified as driveline infections, which are infections that occur where the device's power cord enters the skin (usually in the upper abdomen)<ref name="O'Horo 2018 287–294"/> |
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It is difficult to measure Blood pressure in LVAD patients using standard blood pressure monitoring [[Sphygmomanometer]] and the current practice is to measure by [[Doppler ultrasonography]] in [[Outpatients]] and invasive [[Arterial blood pressure]] monitoring in [[Inpatients]]. <ref>{{Cite journal|last=Castagna|first=Francesco|last2=Stöhr|first2=Eric J.|last3=Pinsino|first3=Alberto|last4=Cockcroft|first4=John R.|last5=Willey|first5=Joshua|last6=Reshad Garan|first6=A.|last7=Topkara|first7=Veli K.|last8=Colombo|first8=Paolo C.|last9=Yuzefpolskaya|first9=Melana|last10=McDonnell|first10=Barry J.|date=2017|title=The Unique Blood Pressures and Pulsatility of LVAD Patients: Current Challenges and Future Opportunities|journal=Current Hypertension Reports|volume=19|issue=10|doi=10.1007/s11906-017-0782-6|issn=1522-6417|pmc=5645430|pmid=29043581}}</ref> |
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VAD-related infection can be caused by a large number of different organisms:<ref>{{cite journal | journal=[[Lancet (journal)|The Lancet Infectious Diseases]] |author=Gordon, RJ |author2=Quagliarello, B |author3=Lowy, FD | title=Ventricular assist device-related infections | year=2006 | volume=6 | issue=7 | pages=426–37 | doi=10.1016/S1473-3099(06)70522-9 | pmid=16790383}}</ref> |
VAD-related infection can be caused by a large number of different organisms:<ref>{{cite journal | journal=[[Lancet (journal)|The Lancet Infectious Diseases]] |author=Gordon, RJ |author2=Quagliarello, B |author3=Lowy, FD | title=Ventricular assist device-related infections | year=2006 | volume=6 | issue=7 | pages=426–37 | doi=10.1016/S1473-3099(06)70522-9 | pmid=16790383}}</ref><ref name="O'Horo 2018 287–294"/> |
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* Gram positive bacteria (''[[Staphylococci]]'', especially ''[[Staphylococcus aureus|Staph. aureus]]'', ''[[Enterococci]]'') |
* Gram positive bacteria (''[[Staphylococci]]'', especially ''[[Staphylococcus aureus|Staph. aureus]]'', ''[[Enterococci]]'') |
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* Gram negative bacteria (''[[Pseudomonas aeruginosa]]'', ''[[Enterobacter]]'' species, ''[[Klebsiella]]'' species) |
* Gram negative bacteria (''[[Pseudomonas aeruginosa]]'', ''[[Enterobacter]]'' species, ''[[Klebsiella]]'' species) |
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* Fungi |
* Fungi, especially ''[[Candida (fungus)|Candida]]'' species |
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Other immune system related problems include [[immunosuppression]]. Some of the [[polyurethane]] components used in the devices cause the deletion of a subset of [[White blood cell|immune cells]] when blood comes in contact with them. This predisposes the patient to [[fungus|fungal]] and some [[virus|viral]] infections necessitating appropriate [[Prophylaxis|prophylactic therapy]].<ref name=holman_infection>{{Cite journal | doi = 10.1016/S0003-4975(03)00479-X | last1 = Holman | first1 = WL | last2 = Rayburn | first2 = BK | last3 = McGiffin | first3 = DC|display-authors=etal | title = Infection in ventricular assist devices: Prevention and treatment | journal = [[The Annals of Thoracic Surgery]] | volume = 75 | issue = 6 Suppl | pages = S48–S57 | year = 2003 | pmid = 12820735 }}</ref> |
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Treatment of VAD-related infection is exceedingly difficult and many patients die of infection despite optimal treatment. Initial treatment should be with broad spectrum antibiotics, but every effort must be made to obtain appropriate samples for culture. A final decision regarding antibiotic therapy must be based on the results of microbiogical cultures.{{Citation needed|date=August 2009}} |
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Considering the multitude of risks and lifestyle modifications associated with ventricular assist device implants,<ref name=Macuccilli>{{cite journal|last1=Marcuccilli|first1=L|last2=Casida|first2=J|last3=Peters|first3=RM|title=Modification of self-concept in patients with a left-ventricular assist device: an initial exploration.|journal=Journal of Clinical Nursing|date=2013|issue=2456–64|pmid=23506318|doi=10.1111/j.1365-2702.2012.04332.x|volume=22|pages=2456–64|url=https://deepblue.lib.umich.edu/bitstream/2027.42/99069/1/jocn4332.pdf|hdl=2027.42/99069|hdl-access=free}}</ref> it is important for prospective patients to be informed prior to decision making.<ref>{{cite journal|last1=Mcillvennan|first1=CK|last2=Allen|first2=LA|last3=Nowels|first3=C|last4=Brieke|first4=A|last5=Cleveland|first5=JC|last6=Matlock|first6=DD|title=Decision making for destination therapy left ventricular assist devices: "there was no choice" versus "I thought about it an awful lot".|journal=[[Circulation (journal)|Circulation: Cardiovascular Quality and Outcomes]] |date=2014|pmid=24823949|doi=10.1161/CIRCOUTCOMES.113.000729|volume=7|issue=3|pages=374–80|pmc=4081474}}</ref> In addition to physician consult, various Internet-based patient directed resources are available to assist in patient education.<ref name=Iacovetto>{{cite journal|last1=Iacovetto|first1=MC|last2=Matlock|first2=DD|last3=Mcillvennan|first3=CK|display-authors=etal|title=Educational resources for patients considering a left ventricular assist device: a cross-sectional review of internet, print, and multimedia materials.|journal=[[Circulation (journal)|Circulation: Cardiovascular Quality and Outcomes]] |date=2014|pmid=25316772|doi=10.1161/CIRCOUTCOMES.114.000892|volume=7|issue=6|pages=905–11|s2cid=7560734 |doi-access=}}</ref><ref name="Matlock Decision Aid">{{cite web|last1=Matlock|first1=DD|last2=Allen|first2=LA|last3=Thompson|first3=JS|last4=Mcilvennan|first4=CK|title=A decision aid for Left Ventricular Assist Device (LVAD) for Destination Therapy A device for patients with advanced heart failure|url=https://patientdecisionaid.org/assets/pdf/lvad_ptda.pdf|date= 31 July 2014|publisher=University of Colorado School of Medicine}}</ref> |
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Other problems include [[immunosuppression]], clotting with resultant stroke, and bleeding secondary to anticoagulation. Some of the [[polyurethane]] components used in the devices cause the deletion of a subset of [[White blood cell|immune cells]] when blood comes in contact with them. This predisposes the patient to [[fungus|fungal]] and some [[virus|viral]] infections necessitating appropriate [[Prophylaxis|prophylactic therapy]].<ref name=holman_infection>{{Cite journal | doi = 10.1016/S0003-4975(03)00479-X | last1 = Holman | first1 = WL | last2 = Rayburn | first2 = BK | last3 = McGiffin | first3 = DC|display-authors=etal | title = Infection in ventricular assist devices: Prevention and treatment | journal = [[The Annals of Thoracic Surgery]] | volume = 75 | issue = 6 Suppl | pages = S48–S57 | year = 2003 | pmid = 12820735 }}</ref> |
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Considering the multitude of risks and lifestyle modifications associated with ventricular assist device implant,<ref name=Macuccilli>{{cite journal|last1=Marcuccilli|first1=L|last2=Casida|first2=J|last3=Peters|first3=RM|title=Modification of self-concept in patients with a left-ventricular assist device: an initial exploration.|journal=Journal of Clinical Nursing|date=2013|issue=2456–64|pmid=23506318|doi=10.1111/j.1365-2702.2012.04332.x|volume=22|pages=2456–64|url=https://deepblue.lib.umich.edu/bitstream/2027.42/99069/1/jocn4332.pdf|hdl=2027.42/99069}}</ref> it is important for prospective patients to be informed prior to decision making.<ref>{{cite journal|last1=Mcillvennan|first1=CK|last2=Allen|first2=LA|last3=Nowels|first3=C|last4=Brieke|first4=A|last5=Cleveland|first5=JC|last6=Matlock|first6=DD|title=Decision making for destination therapy left ventricular assist devices: "there was no choice" versus "I thought about it an awful lot".|journal=[[Circulation (journal)|Circulation: Cardiovascular Quality and Outcomes]] |date=2014|pmid=24823949|doi=10.1161/CIRCOUTCOMES.113.000729|volume=7|pages=374–80|pmc=4081474}}</ref> In addition to physician consult, various Internet-based patient directed resources are available to assist in patient education.<ref name=Iacovetto>{{cite journal|last1=Iacovetto|first1=MC|last2=Matlock|first2=DD|last3=Mcillvennan|first3=CK|display-authors=etal|title=Educational resources for patients considering a left ventricular assist device: a cross-sectional review of internet, print, and multimedia materials.|journal=[[Circulation (journal)|Circulation: Cardiovascular Quality and Outcomes]] |date=2014|pmid=25316772|doi=10.1161/CIRCOUTCOMES.114.000892|volume=7|issue=6|pages=905–11|doi-access=free}}</ref><ref name="Matlock Decision Aid">{{cite web|last1=Matlock|first1=DD|last2=Allen|first2=LA|last3=Thompson|first3=JS|last4=Mcilvennan|first4=CK|title=A decision aid for Left Ventricular Assist Device (LVAD) for Destination Therapy A device for patients with advanced heart failure|url=https://patientdecisionaid.org/assets/pdf/lvad_ptda.pdf|date= 31 July 2014|publisher=University of Colorado School of Medicine}}</ref> |
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== List of implantable VAD devices == |
== List of implantable VAD devices == |
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{{ |
{{update section|date=April 2015}} |
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''This is a partial list and may never be complete''<br /> |
''This is a partial list and may never be complete''<br /> |
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''Referenced additions are welcome'' |
''Referenced additions are welcome'' |
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Line 189: | Line 198: | ||
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| VentrAssist |
| VentrAssist |
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| Ventracor<ref>Ventracor was put into liquidation on 3 July 2009, whereby the company's assets including its intellectual property, data from clinical trials, plant and equipment and residual assets will be put up for sale{{cite news |first= Tony |last= Boyd |title= No Heart |url= http://www.businessspectator.com.au/bs.nsf/Article/No-heart-pd20090703-TL6UR?OpenDocument&src=sph |newspaper= Business Spectator |date= 13 July 2009 | |
| Ventracor<ref>Ventracor was put into liquidation on 3 July 2009, whereby the company's assets including its intellectual property, data from clinical trials, plant and equipment and residual assets will be put up for sale{{cite news |first= Tony |last= Boyd |title= No Heart |url= http://www.businessspectator.com.au/bs.nsf/Article/No-heart-pd20090703-TL6UR?OpenDocument&src=sph |newspaper= Business Spectator |date= 13 July 2009 |access-date=15 September 2009 }}</ref> |
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| Continuous flow driven by a hydrodynamically suspended centrifugal rotor. |
| Continuous flow driven by a hydrodynamically suspended centrifugal rotor. |
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| Approved for use in European Union and Australia. Company declared bankrupt while clinical trials for FDA approval were underway in 2009. Company now dissolved and intellectual property sold to Thoratec. |
| Approved for use in European Union and Australia. Company declared bankrupt while clinical trials for FDA approval were underway in 2009. Company now dissolved and intellectual property sold to Thoratec. |
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Line 196: | Line 205: | ||
|[[www.mitiheart.com]] |
|[[www.mitiheart.com]] |
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| Continuous flow driven by a magnetically suspended centrifugal rotor. |
| Continuous flow driven by a magnetically suspended centrifugal rotor. |
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| Currently in animal testing, recently completed successful 60 |
| Currently in animal testing, recently completed successful 60-day calf implant. |
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|- |
|- |
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| [https://www.chf-solutions.com/aquadex-smartflow-system/ C-Pulse (Now "Aquadex")] |
| [https://www.chf-solutions.com/aquadex-smartflow-system/ C-Pulse (Now "Aquadex")] |
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Line 203: | Line 212: | ||
| Currently available commercially |
| Currently available commercially |
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|- |
|- |
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| [ |
| [https://www.medtronic.com/us-en/patients/treatments-therapies/ventricular-assist-device.html HVAD] |
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| [http://www.heartware.com HeartWare] |
| [http://www.heartware.com HeartWare] (now [https://www.medtronic.com Medtronic]) |
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| Miniature "third generation" device with centrifugal blood path and hydromagnetically suspended rotor that may be placed in the pericardial space. |
| Miniature "third generation" device with centrifugal blood path and hydromagnetically suspended rotor that may be placed in the pericardial space. |
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| Obtained CE Mark for distribution in Europe, January 2009. Obtained FDA approval in the U.S., November 2012. Initiated US BTT trial in October 2008 (completed February 2010) and US DT trial in August 2010 (enrollment completed May 2012). FDA approval for BTT in 2012 and DT in 2017. |
| Obtained CE Mark for distribution in Europe, January 2009. Obtained FDA approval in the U.S., November 2012. Initiated US BTT trial in October 2008 (completed February 2010) and US DT trial in August 2010 (enrollment completed May 2012). FDA approval for BTT in 2012 and DT in 2017. Withdrawn from market in June 2021<ref>{{cite web |url=https://www.fda.gov/news-events/press-announcements/fda-alerts-health-care-providers-stop-new-implants-certain-ventricular-assist-device-system |title=FDA Alerts Health Care Providers to Stop New Implants of Certain Ventricular Assist Device System |author=FDA |website=[[Food and Drug Administration]] |date=3 June 2021 |access-date=8 July 2021 }}</ref> |
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|- |
|- |
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| [http://www.heartware.com/products-technology/technology-pipeline MVAD] |
| [http://www.heartware.com/products-technology/technology-pipeline MVAD] |
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|Pulsatile system includes three major components: Blood pump, cannulae and pneumatic driver (dual drive console or portable VAD driver). |
|Pulsatile system includes three major components: Blood pump, cannulae and pneumatic driver (dual drive console or portable VAD driver). |
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|CE Mark Authorized. Received FDA approval for BTT in 2004. Authorized only for internal implant, not for paracorporeal implant due to reliability issues. |
|CE Mark Authorized. Received FDA approval for BTT in 2004. Authorized only for internal implant, not for paracorporeal implant due to reliability issues. |
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|- |
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|FiVAD |
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|[https://leviticus-cardio.com/ Leviticus Cardio] |
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|Versatile wireless system for LVAD. Allow 6-hour of freedom to the patients |
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|Investigation device, 2 patients trial conduct in Dec 2018 with [https://web.archive.org/web/20070930021005/http://www.jarvikheart.com/basic.asp?id=19 Jarvik 2000] LVAD in Astana by prof Pya.<ref name=":0" /> |
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|} |
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==See also== |
==See also== |
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*[[Intra-aortic balloon pump]] |
* [[Intra-aortic balloon pump]] |
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* [[Pump thrombosis]] |
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==References== |
==References== |
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{{Reflist |
{{Reflist}} |
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==External links== |
==External links== |
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* [http://mylvad.com MyLVAD.com]—Non-branded site with information on various LVADs |
* [http://mylvad.com MyLVAD.com]—Non-branded site with information on various LVADs |
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* [https://patientdecisionaid.org/lvad/ DECIDE-LVAD Patient Decision Aid] - Non-branded site with information on decision making for LVAD |
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{{Intensive care medicine}} |
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{{DEFAULTSORT:Ventricular Assist Device}} |
{{DEFAULTSORT:Ventricular Assist Device}} |
Latest revision as of 05:48, 19 August 2024
Ventricular assist device | |
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MedlinePlus | 007268 |
A ventricular assist device (VAD) is an electromechanical device that provides support for cardiac pump function, which is used either to partially or to completely replace the function of a failing heart. VADs can be used in patients with acute (sudden onset) or chronic (long standing) heart failure, which can occur due to coronary artery disease, atrial fibrillation, valvular disease, and other conditions.[1][2]
Categorization of VADs
[edit]VADs may be used to manage a variety of cardiac diseases and can be categorized based on which ventricle the device is assisting, and whether the VAD will be temporary or permanent.
Ventricular Assistance
First, VADs can be categorized based on whether they are designed to assist the right ventricle (RVAD) or the left ventricle (LVAD) or to both ventricles (BiVAD). The type of VAD implanted depends on the type of underlying heart disease (e.g. patients with right ventricular failure from pulmonary arterial hypertension may require an RVAD, versus those with left ventricular failure from a myocardial infarction may require an LVAD). The LVAD is the most common device applied to a defective heart (it is sufficient in most cases; the right side of the heart is then often able to make use of the heavily increased blood flow), but when the pulmonary arterial resistance is high, then an (additional) right ventricular assist device (RVAD) might be necessary to resolve the problem of cardiac circulation. If both an LVAD and an RVAD are needed a BiVAD is normally used, rather than a separate LVAD and RVAD.[citation needed]
Duration
VADs can further be divided by the duration of their use (i.e. temporary versus permanent). Some VADs are for short-term use,[3] typically for patients recovering from myocardial infarction (heart attack) and for patients recovering from cardiac surgery; some are for long-term use (months to years to perpetuity), typically for patients with advanced heart failure[citation needed]
Temporary use of VADs may vary in scale (e.g. days to months) depending on a patient's condition. Certain types of VADS may be used in patients with signs of acute (sudden onset) heart failure or cardiogenic shock as a result of an infarction, valvular disease, among other causes.[4] In patients with acute signs of heart failure, small percutaneous (introduced to the heart through the skin into a blood vessel rather than through an incision) VADs such as the Impella 5.5, Impella RP, and others can be introduced to either the left or right ventricle (depending on the patient-specific needs) using a wire and that is introduced through the arteries or veins of the neck, axilla, or groin.[5]
Long-term use of VADs may also vary in its scale (i.e. months to permanently). VADs that are intended for long term use are also termed "durable" VADS, due to their design to function for longer periods of time compared to short term VADs (e.g. Impella, etc.). The long-term VADs can be used in a variety of scenarios. First, VADs may be used as bridge to transplantation (BTT) – keeping the patient alive, and in reasonably good condition, and able to await heart transplant outside of the hospital. Other "bridges" include bridge to candidacy (used when a patient has a contraindication to heart transplantation but is expected to improve with the VADs support) , bridge to decision (used to support a patient while their candidacy status is decided), and bridge to recovery (used until a patient’s native heart function improves after which the device would be removed).[6] In some instances, VADs are also used as destination therapy (DT) which indicates that the VAD will remain implanted indefinitely. VADs as destination therapy are used in circumstances where patients are not candidates for transplantation and will thus rely on the VAD for the remainder of their life.[7][8]
Other Cardiac Support Devices
Some devices are designed to support the heart and its various components/function but are not considered VADs, below are some common examples.
Pacemakers and Internal Cardiac Defibrillators (ICDs) – the function of a VAD differs from that of an artificial cardiac pacemaker in that a VAD pumps blood, whereas a pacemaker delivers electrical impulses to the heart muscle.
Total Artificial Heart – VADs are distinct from artificial hearts, which are designed to assume cardiac function, and generally require the removal of the patient's heart.[9]
Extracorporeal Membrane Oxygenation (ECMO) – is a form of mechanical circulatory support typically used in critically ill patients in cardiogenic shock that is established by introducing cannula into the arteries and or veins of the neck, axilla or groin. Generally, a venous cannula pulls deoxygenated blood from the patient's veins into an oxygenating device at the patient's bedside, after which a motor powered pump moves the oxygenated blood is back to the body (either into a vein or the arterial system, typically the aorta). There are different ECMO configurations (venoarterial ECMO, venovenous ECMO, etc.) the end goal remains the same; to oxygenate blood and return it to the body.[10] In this sense, the ECMO circuit bypasses one or both ventricles and is therefore not in contact with the patient's native ventricle and is generally not considered a type of VAD.
Design
[edit]Pumps
[edit]The pumps used in VADs can be divided into two main categories – pulsatile pumps,[11] which mimic the natural pulsing action of the heart, and continuous-flow pumps.[12] Pulsatile VADs use positive displacement pumps.[13][14][15] In some pulsatile pumps (that use compressed air as an energy source[16]), the volume occupied by blood varies during the pumping cycle. If the pump is contained inside the body then a vent tube to the outside air is required.
Continuous-flow VADs are smaller and have proven to be more durable than pulsatile VADs.[17] They normally use either a centrifugal pump or an axial flow pump. Both types have a central rotor containing permanent magnets. Controlled electric currents running through coils contained in the pump housing apply forces to the magnets, which in turn cause the rotors to spin. In the centrifugal pumps, the rotors are shaped to accelerate the blood circumferentially and thereby cause it to move toward the outer rim of the pump, whereas in the axial flow pumps the rotors are more or less cylindrical with blades that are helical, causing the blood to be accelerated in the direction of the rotor's axis.[18]
An important issue with continuous flow pumps is the method used to suspend the rotor. Early versions used solid bearings; however, newer pumps, some of which are approved for use in the EU, use either magnetic levitation ("maglev")[19][20][21] or hydrodynamic suspension.
History
[edit]The first left ventricular assist device (LVAD) system was created by Domingo Liotta at Baylor College of Medicine in Houston in 1962. The first LVAD was implanted in 1963 by Liotta and E. Stanley Crawford. The first successful implantation of an LVAD was completed in 1966 by Liotta along with Dr. Michael E. DeBakey. The patient was a 37-year-old woman, and a paracorporeal (external) circuit was able to provide mechanical support for 10 days after the surgery.[23] The first successful long-term implantation of an LVAD was conducted in 1988 by Dr. William F. Bernhard of Boston Children's Hospital Medical Center and Thermedics, Inc. of Woburn, MA, under a National Institutes of Health (NIH) research contract which developed HeartMate, an electronically controlled assist device. This was funded by a three-year $6.2 million contract to Thermedics and Children's Hospital, Boston, MA, from the National Heart, Lung, and Blood Institute, a program of the NIH.[24] The early VADs emulated the heart by using a "pulsatile" action where blood is alternately sucked into the pump from the left ventricle then forced out into the aorta. Devices of this kind include the HeartMate IP LVAS, which was approved for use in the US by the Food and Drug Administration (FDA) in October 1994. These devices began to gain acceptance in the late 1990s as heart surgeons including Eric Rose, O. H. Frazier and Mehmet Oz began popularizing the concept that patients could live outside the hospital. Media coverage of outpatients with VADs underscored these arguments.[25]
More recent work has concentrated on continuous-flow pumps, which can be roughly categorized as either centrifugal pumps or axial flow impeller driven pumps. These pumps have the advantage of greater simplicity resulting in smaller size and greater reliability. These devices are referred to as second-generation VADs. A side effect is that the user will not have a pulse,[26] or that the pulse intensity will be seriously reduced.[27]
A very different approach in the early stages of development was the use of an inflatable cuff around the aorta. Inflating the cuff contracts the aorta and deflating the cuff allows the aorta to expand – in effect the aorta becomes a second left ventricle. A proposed refinement is to use the patient's skeletal muscle, driven by a pacemaker, to power this device – which would make it truly self-contained. However, a similar operation (cardiomyoplasty) was tried in the 1990s with disappointing results.[citation needed]
At one time Peter Houghton was the longest surviving recipient of a VAD for permanent use. He received an experimental Jarvik 2000 LVAD in June 2000. Since then, he completed a 91-mile charity walk, published two books, lectured widely, hiked in the Swiss Alps and the American West, flew in an ultra-light aircraft, and traveled extensively around the world. He died of acute kidney injury in 2007 at the age of 69.[28][29] Since then, patient Lidia Pluhar has exceeded Houghton's longevity on a VAD, having received a HeartMate II in March 2011 at age 75, and currently continues to use the device. In August 2007 the International Consortium of Circulatory Assist Clinicians (ICCAC) was founded by Anthony "Tony" Martin, a nurse practitioner (NP) and clinical manager of the mechanical circulatory support (MCS) program at Newark Beth Israel Medical Center, Newark, N.J. The ICCAC was developed as a 501c3 organization, dedicated to the development of best practices and education related to the care of individuals requiring MCS as a bridge to heart transplantation or as destination therapy in those individuals who don't meet the criteria for heart transplantation.[30]
Studies and outcomes
[edit]Recent developments
[edit]- In August 2007 The International Consortium of Circulatory Assist Clinicians (ICCAC) was founded by Anthony "Tony" Martin. A nurse practitioner (NP) and clinical manager of the mechanical circulatory support (MCS) program at Newark Beth Israel Medical Center, Newark, N.J..
- In July 2009 in England, surgeons removed a donor heart that had been implanted in a toddler next to her native heart, after her native heart had recovered. This technique suggests mechanical assist device, such as an LVAD, can take some or all the work away from the native heart and allow it time to heal.[31]
- In July 2009, 18-month follow-up results from the HeartMate II Clinical Trial concluded that continuous-flow LVAD provides effective hemodynamic support for at least 18 months in patients awaiting transplantation, with improved functional status and quality of life.[32]
- Heidelberg University Hospital reported in July 2009 that the first HeartAssist5, known as the modern version of the DeBakey VAD, was implanted there. The HeartAssist5 weighs 92 grams, is made of titanium and plastic, and serves to pump blood from the left ventricle into the aorta.[33]
- A phase 1 clinical trial is underway (as of August 2009), consisting of patients with coronary artery bypass grafting and patients in end-stage heart failure who have a left ventricular assist device. The trial involves testing a patch called Anginera which contains cells that secrete hormone-like growth factors stimulating other cells to grow. The patches are seeded with heart muscle cells and then implanted onto the heart with the goal of getting the muscle cells to start communicating with native tissues in a way that allows for regular contractions.[34][35]
- In September 2009, a New Zealand news outlet, Stuff, reported that in another 18 months to two years, a new wireless device will be ready for clinical trial that will power VADs without direct contact. If successful, this may reduce the chance of infection as a result of the power cable through the skin.[36]
- The National Institutes of Health (NIH) awarded a $2.8 million grant to develop a "pulse-less" total artificial heart using two VADs by Micromed, initially created by Michael DeBakey and George Noon. The grant was renewed for a second year of research in August 2009. The total artificial heart was created using two HeartAssist5 VADs, whereby one VAD pumps blood throughout the body and the other circulates blood to and from the lungs.[37]
- HeartWare International announced in August 2009 that it had surpassed 50 implants of their HeartWare Ventricular Assist System in their ADVANCE Clinical Trial, an FDA-approved IDE study. The study is to assess the system as bridge-to-transplantation for patients with end-stage heart failure. The study, Evaluation of the HeartWare LVAD System for the Treatment of Advanced Heart Failure, is a multi-center study that started in May 2009.[38][39]
- On 27 June 2014 Hannover Medical School in Hannover, Germany performed the first human implant of HeartMate III under the direction of Professor Axel Haverich M.D., chief of the Cardiothoracic, Transplantation and Vascular Surgery Department and surgeon Jan Schmitto, M.D., PhD[40]
- On 21 January 2015 a study was published in Journal of American College of Cardiology suggesting that long-term use of LVAD may induce heart regeneration.[41]
- Hall-of-Fame Baseball Player Rod Carew had congestive heart failure and was fitted with a HeartMate II. He struggled with wearing the equipment, so he joined efforts to help supply the most helpful wear to assist the HeartMate II and HeartMate III.[42]
- In December 2018, two clinical cases were performed in Kazakhstan and a fully wireless LVAD system of Jarvik 2000 combine with Leviticus Cardio FiVAD (Fully Implantable Ventricular Assist Device) were implanted in humans. The Wireless power transfer technology based on technique called Coplanar Energy Transfer (CET) which is capable of transferring energy from an external transmitting coil to a small receiving coil that is implanted in the human body. In the early postoperative phase, CET operation was accomplished as expected in both patients, which powered the pump and maintained the battery charged to allow medical and nursing procedures. The Leviticus Cardio FiVAD System with wireless, coplanar energy transfer technology which ameliorates infection risk by driveline elimination while providing successful energy transmission allowing for a substantial (approximately 6 hours) unholstered support of the LVAD.[43]
- On June 3, 2021, Medtronic issued an urgent medical device notice stating that their HVAD devices should no longer be implanted due to higher rates of neurological events and mortality with the HVAD vs. other available devices [44]
The majority of VADs on the market today are somewhat bulky. The smallest device approved by the FDA, the HeartMate II, weighs about 1 pound (0.45 kg) and measures 3 inches (7.6 cm). This has proven particularly important for women and children, for whom alternatives would have been too large.[45] As of 2017, HeartMate III has been approved by the FDA. It is smaller than its predecessor HeartMate II and uses a full maglev impeller instead of the cup-and-ball bearing system found in HeartMate II.[46]
The HeartWare HVAD works similarly to the VentrAssist—albeit much smaller and not requiring an abdominal pocket to be implanted into. The device has obtained CE Mark in Europe, and FDA approval in the U.S. The HeartWare HVAD could be implanted through limited access without sternotomy, however in 2021 Medtronic discontinued the device.[47][44]
In a small number of cases left ventricular assist devices, combined with drug therapy, have enabled the heart to recover sufficiently for the device to be able to be removed (explanted).[7][8] Several surgical approaches, including interventional decommissioning, off-pump explantation using a custom-made plug and complete LVAD removal through redo sternotomy, have been described with a 5-year survival of up to 80%.[48]
HeartMate II LVAD pivotal study
[edit]A series of studies involving the use of the HeartMate II LVAD have proven useful in establishing the viability and risks of using LVADs for bridge-to-transplantation and destination therapy.
- The HeartMate II pivotal trial began in 2005 and included the evaluation of HeartMate II for two indications: Bridge to transplantation (BTT) and destination therapy (DT), or long-term, permanent support. Thoratec Corp. announced that this was the first time the FDA had approved a clinical trial to include both indications in one protocol.[49][50][51]
- A multicenter study in the United States from 2005 to 2007 with 113 patients (of which 100 reported principal outcomes) showed that significant improvements in function were prevalent after three months, and a survival rate of 68% after twelve months.[52]
- Based on one-year follow up data from the first 194 patients enrolled in the trial, the FDA approved HeartMate II for bridge-to-transplantation. The trial provided clinical evidence of improved survival rates and quality of life for a broad range of patients.[53][54]
- Eighteen-month follow up data on 281 patients who had either reached the study end-point or completed 18 months of post-operative follow-up showed improved survival, less frequent adverse events and greater reliability with continuous flow LVADS compared to pulsatile flow devices. Of the 281 patients, 157 patients had undergone transplant, 58 patients were continuing with LVADs in their body and seven patients had the LVAD removed because their heart recovered; the remaining 56 had died. The results showed that the patients' NYHA Class of heart failure had significantly improved after six months of LVAD support compared to the pre-LVAD baseline. Although this trial involved bridge-to-transplant indication, the results provide early evidence that continuous flow LVADs have advantages in terms of durability and reliability for patients receiving mechanical support for destination therapy.[55]
- Following the FDA approval of HeartMate II LVAD for bridge-to-transplantation purposes, a post-approval ("registry") study was undertaken to assess the efficacy of the device in a commercial setting. The study found that the device improved outcomes, both compared to other LVAD treatments and baseline patients. Specifically, HeartMate II patients showed lower creatinine levels, 30-day survival rates were considerably higher at 96%, and 93% reached successful outcomes (transplant, cardiac recovery, or long-term LVAD).[56]
HARPS
[edit]The Harefield Recovery Protocol Study (HARPS) is a clinical trial to evaluate whether advanced heart failure patients requiring VAD support can recover sufficient myocardial function to allow device removal (known as explantation). HARPS combines an LVAD (the HeartMate XVE) with conventional oral heart failure medications, followed by the novel β2 agonist clenbuterol. This opens the possibility that some advanced heart failure patients may forgo heart transplantation.[57]
REMATCH
[edit]The REMATCH (Randomized Evaluation of Mechanical Assistance for the Treatment of Congestive Heart Failure) clinical trial began in May 1998 and ran through July 2001 in 20 cardiac transplant centers around the USA. The trial was designed to compare long-term implantation of left ventricular assist devices with optimal medical management for patients with end-stage heart failure who require, but do not qualify to receive cardiac transplantation. As a result of the clinical outcomes, the device received FDA approval for both indications, in 2001 and 2003, respectively.[58]
According to a retrospective cohort study comparing patients treated with a left ventricular assist device versus inotrope therapy while awaiting heart transplantation, the group treated with LVAD had improved clinical and metabolic function at the time of transplant with better blood pressure, sodium, blood urea nitrogen, and creatinine. After transplant, 57.7% of the inotrope group had kidney failure versus 16.6% in the LVAD group; 31.6% of the inotrope group had right heart failure versus 5.6% in the LVAD group; and event-free survival was 15.8% in the inotrope group versus 55.6% in the LVAD group.[59]
Complications and side effects
[edit]There are a number of potential risks associated with VADs. The most common of these are bleeding events, stroke, pump thrombosis, and infections.[60]
Bleeding
Because the VADs generally result in blood flowing over a non-biologic surface (e.g. metal, synthetic polymers, etc.) this can result in formation of blood clots, also referred to as thrombosis. Due to these clotting abnormalities, anticoagulation medications are used to decrease the risk of thrombosis. One device, the HeartMate XVE, is designed with a biologic surface derived from fibrin and does not require long term anticoagulation (except aspirin); unfortunately, this biologic surface may also predispose the patient to infection through selective reduction of certain types of leukocytes, however this device was phased out of use starting in 2009 in favor of newer devices.[61][62]
Due to the use of anticoagulation, bleeding is the most common postoperative early complication after implantation or explantation of VADs, necessitating reoperation in up to 60% of recipients.[63][64] Most commonly bleeding occurs in the gastrointestinal tract resulting in dark or bright red stools,[65] however if trauma to the head occurs, intracranial bleeding may also occur.[66] Bleeding events may require massive blood transfusions and incur certain risks including infection, pulmonary insufficiency, increased costs, right heart failure, allosensitization, and viral transmission, which can prove fatal or preclude transplantation.[64] When bleeding occurs, it impacts the one year Kaplan-Meier mortality.[63] In addition to complexity of the patient population and the complexity of these procedures contributing to bleeding, the devices themselves may contribute to the severe coagulopathy that can ensue when these devices are implanted.[67]
Ischemic Stroke and Pump Thrombosis
In patients with VADs, ischemic strokes and pump thrombosis occur when there is inadequate anticoagulation to counter act the blood's tendency to form blood clots when exposed to the foreign materials in a VAD. Stroke risk varies based on the type of VAD in place and other risk factors.[60] Both atrial fibriliation and high blood pressure may increase risk of stroke and high blood pressure can increase a patient's risk of stroke in the setting of VAD use.[68] However, it is difficult to measure blood pressure in LVAD patients using standard blood pressure monitoring and the current practice is to measure by Doppler ultrasonography in outpatients and invasive arterial blood pressure monitoring in inpatients.[69]
Infections
Infections in VAD patients occur because the artificial surfaces of the devices serve as a surface for bacterial and or fungal growth.[70] Most infections are classified as driveline infections, which are infections that occur where the device's power cord enters the skin (usually in the upper abdomen)[70]
VAD-related infection can be caused by a large number of different organisms:[71][70]
- Gram positive bacteria (Staphylococci, especially Staph. aureus, Enterococci)
- Gram negative bacteria (Pseudomonas aeruginosa, Enterobacter species, Klebsiella species)
- Fungi, especially Candida species
Other immune system related problems include immunosuppression. Some of the polyurethane components used in the devices cause the deletion of a subset of immune cells when blood comes in contact with them. This predisposes the patient to fungal and some viral infections necessitating appropriate prophylactic therapy.[72]
Considering the multitude of risks and lifestyle modifications associated with ventricular assist device implants,[73] it is important for prospective patients to be informed prior to decision making.[74] In addition to physician consult, various Internet-based patient directed resources are available to assist in patient education.[75][76]
List of implantable VAD devices
[edit]This section needs to be updated.(April 2015) |
This is a partial list and may never be complete
Referenced additions are welcome
Device | Manufacturer | Type | Approval Status as of July 2010 |
---|---|---|---|
HeartAssist5 | ReliantHeart | Continuous flow driven by an axial flow rotor. | Approved for use in the European Union. The child version is approved by the FDA for use in children in USA. Undergoing clinical trials in USA for FDA approval. |
Novacor | World Heart | Pulsatile. | Was approved for use in North America, European Union and Japan. Now defunct and no longer supported by the manufacturer. (HeartWare completed acquisition August 2012) |
HeartMate XVE | Thoratec | Pulsatile | FDA approval for BTT in 2001 and DT in 2003. CE Mark Authorized. Rarely used anymore due to reliability concerns. |
HeartMate II | Thoratec | Rotor driven continuous axial flow, ball and cup bearings. | Approved for use in North America and EU. CE Mark Authorized. FDA approval for BTT in April 2008. Recently approved by FDA in the US for Destination Therapy (as at January 2010). |
HeartMate III | Thoratec | Continuous flow driven by a magnetically suspended axial flow rotor. | Pivotal trials for HeartMate III started in 2014 and supported with CarewMedicalWear. FDA approval for BTT in 2017 |
Incor | Berlin Heart | Continuous flow driven by a magnetically suspended axial flow rotor. | Approved for use in European Union. Used on humanitarian approvals on a case-by-case basis in the US. Entered clinical trials in the US in 2009. |
Excor Pediatric | Berlin Heart | External membrane pump device designed for children. | Approved for use in European Union. FDA granted Humanitarian Device Exemption for US in December 2011. |
Jarvik 2000 | Jarvik Heart | Continuous flow, axial rotor supported by ceramic bearings. | Currently used in the United States as a bridge to heart transplant under an FDA-approved clinical investigation. In Europe, the Jarvik 2000 has earned CE Mark certification for both bridge-to-transplant and lifetime use. Child version currently being developed. |
MicroMed DeBakey VAD | MicroMed | Continuous flow driven by axial rotor supported by ceramic bearings. | Approved for use in the European Union. The child version is approved by the FDA for use in children in USA. Undergoing clinical trials in USA for FDA approval. |
VentrAssist | Ventracor[77] | Continuous flow driven by a hydrodynamically suspended centrifugal rotor. | Approved for use in European Union and Australia. Company declared bankrupt while clinical trials for FDA approval were underway in 2009. Company now dissolved and intellectual property sold to Thoratec. |
MTIHeartLVAD | www.mitiheart.com | Continuous flow driven by a magnetically suspended centrifugal rotor. | Currently in animal testing, recently completed successful 60-day calf implant. |
C-Pulse (Now "Aquadex") | Sunshine Heart (Now "CHF Solutions") | Pulsatile, driven by an inflatable cuff around the aorta. | Currently available commercially |
HVAD | HeartWare (now Medtronic) | Miniature "third generation" device with centrifugal blood path and hydromagnetically suspended rotor that may be placed in the pericardial space. | Obtained CE Mark for distribution in Europe, January 2009. Obtained FDA approval in the U.S., November 2012. Initiated US BTT trial in October 2008 (completed February 2010) and US DT trial in August 2010 (enrollment completed May 2012). FDA approval for BTT in 2012 and DT in 2017. Withdrawn from market in June 2021[78] |
MVAD | HeartWare | HeartWare's MVAD Pump is a development-stage miniature ventricular assist device, approximately one-third the size of HeartWare's HVAD pump. | HeartWare Completed GLP Studies (September 2011). |
DuraHeart | Terumo | Magnetically levitated centrifugal pump. | CE approved, US FDA trials underway as at January 2010. |
Thoratec PVAD (Paracorporeal Ventricular Assist Device) | Thoratec | Pulsatile system includes three major components: Blood pump, cannulae and pneumatic driver (dual drive console or portable VAD driver). | CE Mark Authorized. Received FDA approval for BTT in 1995 and for post-cardiotomy recovery (open heart surgery) in 1998. |
IVAD—Implantable Ventricular Assist Device | Thoratec | Pulsatile system includes three major components: Blood pump, cannulae and pneumatic driver (dual drive console or portable VAD driver). | CE Mark Authorized. Received FDA approval for BTT in 2004. Authorized only for internal implant, not for paracorporeal implant due to reliability issues. |
FiVAD | Leviticus Cardio | Versatile wireless system for LVAD. Allow 6-hour of freedom to the patients | Investigation device, 2 patients trial conduct in Dec 2018 with Jarvik 2000 LVAD in Astana by prof Pya.[43] |
See also
[edit]References
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External links
[edit]- MyLVAD.com—Non-branded site with information on various LVADs
- DECIDE-LVAD Patient Decision Aid - Non-branded site with information on decision making for LVAD