4.7 Review

New Insights in Mechanisms and Therapeutics for Short- and Long-Term Impacts of Hepatic Ischemia Reperfusion Injury Post Liver Transplantation

Journal

Publisher

MDPI
DOI: 10.3390/ijms22158210

Keywords

liver ischemia reperfusion injury; inflammation; immune responses; metabolism; therapeutic strategies

Funding

  1. Research Grant Council, Hong Kong [GRF: 17124219, 17122517, 17159616, 17115515]
  2. Theme-based Research Scheme [TRS: T12-703/19R]

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Liver transplantation is effective for end-stage liver disease patients, but may lead to hepatic ischemia reperfusion injury (IRI) causing acute inflammation, graft dysfunction, acute rejection, chronic rejection, cancer recurrence, and fibrogenesis. Understanding the mechanisms of inflammation and immune activation during IRI, as well as developing therapeutic strategies, is crucial for improving transplant outcomes.
Liver transplantation has been identified as the most effective treatment for patients with end-stage liver diseases. However, hepatic ischemia reperfusion injury (IRI) is associated with poor graft function and poses a risk of adverse clinical outcomes post transplantation. Cell death, including apoptosis, necrosis, ferroptosis and pyroptosis, is induced during the acute phase of liver IRI. The release of danger-associated molecular patterns (DAPMs) and mitochondrial dysfunction resulting from the disturbance of metabolic homeostasis initiates graft inflammation. The inflammation in the short term exacerbates hepatic damage, leading to graft dysfunction and a higher incidence of acute rejection. The subsequent changes in the graft immune environment due to hepatic IRI may result in chronic rejection, cancer recurrence and fibrogenesis in the long term. In this review, we mainly focus on new mechanisms of inflammation initiated by immune activation related to metabolic alteration in the short term during liver IRI. The latest mechanisms of cancer recurrence and fibrogenesis due to the long-term impact of inflammation in hepatic IRI is also discussed. Furthermore, the development of therapeutic strategies, including ischemia preconditioning, pharmacological inhibitors and machine perfusion, for both attenuating acute inflammatory injury and preventing late-phase disease recurrence, will be summarized in the context of clinical, translational and basic research.

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