A cardioprotective preservation strategy employing ex vivo heart perfusion facilitates successful transplant of donor hearts after cardiocirculatory death

Christopher W White; Ayyaz Ali; Devin Hasanally; Bo Xiang; Yun Li; Paul Mundt; Matthew Lytwyn; Simon Colah; Julianne Klein; Amir Ravandi; Rakesh C Arora; Trevor W Lee; Larry Hryshko; Stephen Large; Ganghong Tian; Darren H Freed

doi:10.1016/j.healun.2013.04.016

A cardioprotective preservation strategy employing ex vivo heart perfusion facilitates successful transplant of donor hearts after cardiocirculatory death

J Heart Lung Transplant. 2013 Jul;32(7):734-43. doi: 10.1016/j.healun.2013.04.016.

Authors

Christopher W White¹, Ayyaz Ali, Devin Hasanally, Bo Xiang, Yun Li, Paul Mundt, Matthew Lytwyn, Simon Colah, Julianne Klein, Amir Ravandi, Rakesh C Arora, Trevor W Lee, Larry Hryshko, Stephen Large, Ganghong Tian, Darren H Freed

Affiliation

¹ Cardiac Sciences Program, University of Manitoba, St Boniface Hospital, Winnipeg, Manitoba, Canada.

PMID: 23796155
DOI: 10.1016/j.healun.2013.04.016

Abstract

Background: Ex vivo heart perfusion (EVHP) has been proposed as a means to facilitate the resuscitation of donor hearts after cardiocirculatory death (DCD) and increase the donor pool. However, the current approach to clinical EVHP may exacerbate myocardial injury and impair function after transplant. Therefore, we sought to determine if a cardioprotective EVHP strategy that eliminates myocardial exposure to hypothermic hyperkalemia cardioplegia and minimizes cold ischemia could facilitate successful DCD heart transplantation.

Methods: Anesthetized pigs sustained a hypoxic cardiac arrest and a 15-minute warm ischemic standoff period. Strategy 1 hearts (S1, n = 9) underwent initial reperfusion with a cold hyperkalemic cardioplegia, normothermic EVHP, and transplantation after a cold hyperkalemic cardioplegic arrest (current EVHP strategy). Strategy 2 hearts (S2, n = 8) underwent initial reperfusion with a tepid adenosine-lidocaine cardioplegia, normothermic EVHP, and transplantation with continuous myocardial perfusion (cardioprotective EVHP strategy).

Results: At completion of EVHP, S2 hearts exhibited less weight gain (9.7 ± 6.7 [S2] vs 21.2 ± 6.7 [S1] g/hour, p = 0.008) and less troponin-I release into the coronary sinus effluent (4.2 ± 1.3 [S2] vs 6.3 ± 1.5 [S1] ng/ml; p = 0.014). Mass spectrometry analysis of oxidized pleural in post-transplant myocardium revealed less oxidative stress in S2 hearts. At 30 minutes after wean from cardiopulmonary bypass, post-transplant systolic (pre-load recruitable stroke work: 33.5 ± 1.3 [S2] vs 19.7 ± 10.9 [S1], p = 0.043) and diastolic (isovolumic relaxation constant: 42.9 ± 6.7 [S2] vs 65.2 ± 21.1 [S1], p = 0.020) function were superior in S2 hearts.

Conclusion: In this experimental model of DCD, an EVHP strategy using initial reperfusion with a tepid adenosine-lidocaine cardioplegia and continuous myocardial perfusion minimizes myocardial injury and improves short-term post-transplant function compared with the current EVHP strategy using cold hyperkalemic cardioplegia before organ procurement and transplantation.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Adenosine / therapeutic use*
Animals
Death
Female
Heart Arrest, Induced*
Heart Transplantation*
Lidocaine / therapeutic use*
Organ Preservation / methods*
Perfusion
Swine

Substances

Lidocaine
Adenosine