Ex Situ Liver Machine Perfusion: The Impact of Fresh Frozen Plasma

Qiang Liu; Ahmed Hassan; Daniele Pezzati; Basem Soliman; Laura Lomaglio; Patrick Grady; Laurent Del Angel Diaz; Andrea Simioni; Shana Maikhor; John Etterling; Giuseppe D'Amico; Giuseppe Iuppa; Teresa Diago Uso; Koji Hashimoto; Federico Aucejo; Masato Fujiki; Bijan Eghtesad; Kazunari Sasaki; Choon Hyuck David Kwon; Jacek Cywinski; Samuel Irefin; Ana Bennett; William Baldwin; Charles Miller; Cristiano Quintini

doi:10.1002/lt.25668

Ex Situ Liver Machine Perfusion: The Impact of Fresh Frozen Plasma

Liver Transpl. 2020 Feb;26(2):215-226. doi: 10.1002/lt.25668.

Authors

Qiang Liu¹, Ahmed Hassan¹, Daniele Pezzati¹, Basem Soliman¹, Laura Lomaglio¹, Patrick Grady², Laurent Del Angel Diaz¹, Andrea Simioni¹, Shana Maikhor¹, John Etterling¹, Giuseppe D'Amico¹, Giuseppe Iuppa¹, Teresa Diago Uso¹, Koji Hashimoto¹, Federico Aucejo¹, Masato Fujiki¹, Bijan Eghtesad¹, Kazunari Sasaki¹, Choon Hyuck David Kwon¹, Jacek Cywinski³, Samuel Irefin³, Ana Bennett¹, William Baldwin⁴, Charles Miller¹, Cristiano Quintini¹

Affiliations

¹ Transplantation Center, Department of Surgery, Digestive Disease Institute, Cleveland Clinic, Cleveland, OH.
² Perfusion Services, Heart and Vascular Institute, Cleveland Clinic, Cleveland, OH.
³ Anesthesiology Institute, Cleveland Clinic, Cleveland, OH.
⁴ Inflammation and Immunity Department, Lerner Research Institute, Cleveland Clinic, Cleveland, OH.

PMID: 31642164
DOI: 10.1002/lt.25668

Abstract

The primary aim of this single-center, phase 1 exploratory study was to investigate the safety, feasibility, and impact on intrahepatic hemodynamics of a fresh frozen plasma (FFP)-based perfusate in ex situ liver normothermic machine perfusion (NMP) preservation. Using an institutionally developed perfusion device, 21 livers (13 donations after brain death and 8 donations after circulatory death) were perfused for 3 hours 21 minutes to 7 hours 52 minutes and successfully transplanted. Outcomes were compared in a 1:4 ratio to historical control patients matched according to donor and recipient characteristics and preservation time. Perfused livers presented a very low resistance state with high flow during ex situ perfusion (arterial and portal flows 340 ± 150 and 890 ± 70 mL/minute/kg liver, respectively). This hemodynamic state was maintained even after reperfusion as demonstrated by higher arterial flow observed in the NMP group compared with control patients (220 ± 120 versus 160 ± 80 mL/minute/kg liver, P = 0.03). The early allograft dysfunction (EAD) rate, peak alanine aminotransferase (ALT), and peak aspartate aminotransferase (AST) levels within 7 days after transplantation were lower in the NMP group compared with the control patients (EAD 19% versus 46%, P = 0.02; peak ALT 363 ± 318 versus 1021 ± 999 U/L, P = 0.001; peak AST 1357 ± 1492 versus 2615 ± 2541 U/L, P = 0.001 of the NMP and control groups, respectively). No patient developed ischemic type biliary stricture. One patient died, and all other patients are alive and well at a follow-up of 12-35 months. No device-related adverse events were recorded. In conclusion, with this study, we showed that ex situ NMP of human livers can be performed safely and effectively using a noncommercial device and an FFP-based preservation solution. Future studies should further investigate the impact of an FFP-based perfusion solution on liver hemodynamics during ex situ normothermic machine preservation.

MeSH terms

Humans
Liver
Liver Transplantation* / adverse effects
Organ Preservation*
Perfusion
Plasma