Transplantation Direct (Aug 2024)

Optimizing DCD Liver Grafts With Prolonged Warm Ischemic Time Using Stabilized Plasmin in a Static Cold Storage Orthotopic Rat Liver Transplant Model

  • Riley Kahan, BS,
  • Nader Abraham, MD,
  • Min Zhang, MD,
  • Valery Novokhatny, PhD,
  • Isaac Alderete, BS,
  • Paul Cray, PhD,
  • Fengming Chen, MD, PhD,
  • Qimeng Gao, MD,
  • Greta Cywinska, BS,
  • Ryan Neill,
  • Kentaro Nakata, MD, PhD,
  • Ahmed Hassan, MD,
  • Caroline Rush, BS,
  • Jude Penaflor, BS,
  • Justin J. Pollara, PhD,
  • Matthew G. Hartwig, MD,
  • Benjamin Hughes, PhD,
  • Andrew S. Barbas, MD

DOI
https://doi.org/10.1097/TXD.0000000000001665
Journal volume & issue
Vol. 10, no. 8
p. e1665

Abstract

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Background. The clinical success of liver transplantation has led to increased demand, requiring further expansion of the donor pool. Therapeutic interventions to optimize organs from donation after circulatory death (DCD) have significant potential to mitigate the organ shortage. Dysfunction in DCD liver grafts is mediated by microvascular thrombosis during the warm ischemic period, and strategies that reduce this thrombotic burden may improve graft function. We hypothesized that the administration of the fibrinolytic enzyme plasmin to the donor organ during the cold storage period would reduce the thrombotic burden and improve DCD liver graft function. Methods. In 2 separate cohorts, 32 syngeneic orthotopic rat liver transplants were performed in Lewis rats. Livers were procured from donors with 45 min of warm ischemic injury. Liver grafts were flushed with histidine-tryptophan-ketoglutarate preservation solution mixed with either plasmin (experimental group) or albumin (control group). All investigators were blinded to treatment group. After preparing the liver for implant using a modified cuff technique, the liver was stored for 1 h by static cold storage at 4 °C. Immediately before implantation, the liver graft was flushed, and this effluent was analyzed for fibrin degradation products to determine graft clot burden. Twenty-four hours following transplantation, animals were euthanized, and samples were collected. Results. Recipient survival was significantly higher for DCD liver grafts treated with plasmin compared with control. Moreover, histology of liver graft tissue immediately before implant reflected significantly reduced congestion in plasmin-treated livers (score, mean ± SD: 0.73 ± 0.59 versus 1.12 ± 0.48; P = 0.0456). The concentration of fibrin degradation products in the final flush before implantation was significantly reduced in plasmin-treated livers (743 ± 136 versus 10 919 ± 4642 pg/mL; P = 0.0001), reflecting decreased clot burden in the graft. Conclusions. The present study demonstrates that plasmin improves survival and may reduce thrombotic burden in DCD liver grafts with prolonged warm ischemic injury, meriting further study.