Hepatology Communications (May 2022)

MutT Homolog 1 Inhibitor Karonudib Attenuates Autoimmune Hepatitis by Inhibiting DNA Repair in Activated T Cells

  • Yong Chen,
  • Xiangwei Hua,
  • Bingyuan Huang,
  • Stella Karsten,
  • Zhengrui You,
  • Bo Li,
  • You Li,
  • Yikang Li,
  • Jubo Liang,
  • Jun Zhang,
  • Yiran Wei,
  • Ruiling Chen,
  • Zhuwan Lyu,
  • Xiao Xiao,
  • Min Lian,
  • Jue Wei,
  • Jingyuan Fang,
  • Qi Miao,
  • Qixia Wang,
  • Ulrika Warpman Berglung,
  • Ruqi Tang,
  • Thomas Helleday,
  • Xiong Ma

DOI
https://doi.org/10.1002/hep4.1862
Journal volume & issue
Vol. 6, no. 5
pp. 1016 – 1031

Abstract

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Autoimmune hepatitis (AIH) is an inflammatory liver disease driven by the hyperactivation of various intrahepatic antigen‐specific T cells due to a breach of immune tolerance. Studies in immunometabolism demonstrate that activated T cells harbor increased levels of reactive oxygen species that cause oxidative DNA damage. In this study, we assessed the potential of DNA damage repair enzyme MutT homolog 1 (MTH1) as a therapeutic target in AIH and karonudib as a novel drug for patients with AIH. We report herein that MTH1 expression was significantly increased in liver samples from patients with AIH compared to patients with chronic hepatitis B and nonalcoholic fatty liver disease and from healthy controls. In addition, the expression of MTH1 was positively correlated with AIH disease severity. We further found abundant T cells that expressed MTH1 in AIH. Next, we found that karonudib significantly altered T‐cell receptor signaling in human T cells and robustly inhibited proliferation of human T cells in vitro. Interestingly, our data reflected a preferential inhibition of DNA damage repair in activated T cells by karonudib. Moreover, MTH1 was required to develop liver inflammation and damage because specific deletion of MTH1 in T cells ameliorated liver injury in the concanavalin A (Con A)‐induced hepatitis model by inhibiting T‐cell activation and proliferation. Lastly, we validated the protective effect of karonudib on the Con A‐induced hepatitis model. Conclusion: MTH1 functions as a critical regulator in the development of AIH, and its inhibition in activated T cells reduces liver inflammation and damage.