Hepatic ferroptosis plays an important role as the trigger for initiating inflammation in nonalcoholic steatohepatitis

Shinya Tsurusaki; Yuichi Tsuchiya; Tomoko Koumura; Misaki Nakasone; Taro Sakamoto; Masaki Matsuoka; Hirotaka Imai; Cindy Kok; Hitoshi Okochi; Hiroyasu Nakano; Atsushi Miyajima; Minoru Tanaka

doi:10.1038/s41419-019-1678-y

Hepatic ferroptosis plays an important role as the trigger for initiating inflammation in nonalcoholic steatohepatitis

Shinya Tsurusaki(National Center for Global Health and Medicine), Yuichi Tsuchiya(Toho University), Tomoko Koumura(Kitasato University), Misaki Nakasone(Kitasato University), Taro Sakamoto(Kitasato University), Masaki Matsuoka(Kitasato University), Hirotaka Imai(Kitasato University), Cindy Kok(National Center for Global Health and Medicine), Hitoshi Okochi(National Center for Global Health and Medicine), Hiroyasu Nakano(Toho University), Atsushi Miyajima(The University of Tokyo), Minoru Tanaka(National Center for Global Health and Medicine)

Cell Death and Disease

June 17, 2019

10.1038/s41419-019-1678-y

Cited by 505Open Access

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Abstract

Nonalcoholic steatohepatitis (NASH) is a metabolic liver disease that progresses from simple steatosis to the disease state of inflammation and fibrosis. Previous studies suggest that apoptosis and necroptosis may contribute to the pathogenesis of NASH, based on several murine models. However, the mechanisms underlying the transition of simple steatosis to steatohepatitis remain unclear, because it is difficult to identify when and where such cell deaths begin to occur in the pathophysiological process of NASH. In the present study, our aim is to investigate which type of cell death plays a role as the trigger for initiating inflammation in fatty liver. By establishing a simple method of discriminating between apoptosis and necrosis in the liver, we found that necrosis occurred prior to apoptosis at the onset of steatohepatitis in the choline-deficient, ethionine-supplemented (CDE) diet model. To further investigate what type of necrosis is involved in the initial necrotic cell death, we examined the effect of necroptosis and ferroptosis inhibition by administering inhibitors to wild-type mice in the CDE diet model. In addition, necroptosis was evaluated using mixed lineage kinase domain-like protein (MLKL) knockout mice, which is lacking in a terminal executor of necroptosis. Consequently, necroptosis inhibition failed to block the onset of necrotic cell death, while ferroptosis inhibition protected hepatocytes from necrotic death almost completely, and suppressed the subsequent infiltration of immune cells and inflammatory reaction. Furthermore, the amount of oxidized phosphatidylethanolamine, which is involved in ferroptosis pathway, was increased in the liver sample of the CDE diet-fed mice. These findings suggest that hepatic ferroptosis plays an important role as the trigger for initiating inflammation in steatohepatitis and may be a therapeutic target for preventing the onset of steatohepatitis.

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