| Literature DB >> 31909544 |
Naoya Yamada1,2, Tadayoshi Karasawa1, Taiichi Wakiya3, Ai Sadatomo1, Homare Ito1, Ryo Kamata1, Sachiko Watanabe1, Takanori Komada1, Hiroaki Kimura1, Yukihiro Sanada2, Yasunaru Sakuma2, Koichi Mizuta4, Nobuhiko Ohno5,6, Naohiro Sata2, Masafumi Takahashi1.
Abstract
Hepatic ischemia-reperfusion (I/R) injury is a major problem in liver transplantation (LT). Although hepatocyte cell death is the initial event in hepatic I/R injury, the underlying mechanism remains unclear. In the present study, we retrospectively analyzed the clinical data of 202 pediatric living donor LT and found that a high serum ferritin level, a marker of iron overload, of the donor is an independent risk factor for liver damage after LT. Since ferroptosis has been recently discovered as an iron-dependent cell death that is triggered by a loss of cellular redox homeostasis, we investigated the role of ferroptosis in a murine model of hepatic I/R injury, and found that liver damage, lipid peroxidation, and upregulation of the ferroptosis marker Ptgs2 were induced by I/R, and all of these manifestations were markedly prevented by the ferroptosis-specific inhibitor ferrostatin-1 (Fer-1) or α-tocopherol. Fer-1 also inhibited hepatic I/R-induced inflammatory responses. Furthermore, hepatic I/R injury was attenuated by iron chelation by deferoxamine and exacerbated by iron overload with a high iron diet. These findings demonstrate that iron overload is a novel risk factor for hepatic I/R injury in LT, and ferroptosis contributes to the pathogenesis of hepatic I/R injury.Entities:
Keywords: cell death; liver transplantation/hepatology; liver transplantation: living donor; translational research/science
Mesh:
Year: 2020 PMID: 31909544 DOI: 10.1111/ajt.15773
Source DB: PubMed Journal: Am J Transplant ISSN: 1600-6135 Impact factor: 8.086