Frontiers in Immunology (Mar 2024)

JNK signaling mediates acute rejection via activating autophagy of CD8+ T cells after liver transplantation in rats

  • Xiaowen Wang,
  • Xiaowen Wang,
  • Wenfeng Zhu,
  • Wenfeng Zhu,
  • Haoqi Chen,
  • Haoqi Chen,
  • Xuejiao Li,
  • Wenjie Zheng,
  • Wenjie Zheng,
  • Yuan Zhang,
  • Ning Fan,
  • Xiaolong Chen,
  • Genshu Wang

DOI
https://doi.org/10.3389/fimmu.2024.1359859
Journal volume & issue
Vol. 15

Abstract

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BackgroundAcute rejection (AR) after liver transplantation (LT) remains an important factor affecting the prognosis of patients. CD8+ T cells are considered to be important regulatory T lymphocytes involved in AR after LT. Our previous study confirmed that autophagy mediated AR by promoting activation and proliferation of CD8+ T cells. However, the underlying mechanisms regulating autophagy in CD8+ T cells during AR remain unclear.MethodsHuman liver biopsy specimens of AR after orthotopic LT were collected to assess the relationship between JNK and CD8+ T cells autophagy. The effect of JNK inhibition on CD8+ T cells autophagy and its role in AR were further examined in rats. Besides, the underlying mechanisms how JNK regulated the autophagy of CD8+ T cells were further explored.ResultsThe expression of JNK is positive correlated with the autophagy level of CD8+ T cells in AR patients. And similar findings were obtained in rats after LT. Further, JNK inhibitor remarkably inhibited the autophagy of CD8+ T cells in rat LT recipients. In addition, administration of JNK inhibitor significantly attenuated AR injury by promoting the apoptosis and downregulating the function of CD8+ T cells. Mechanistically, JNK may activate the autophagy of CD8+ T cells through upregulating BECN1 by inhibiting the formation of Bcl-2/BECN1 complex.ConclusionJNK signaling promoted CD8+ T cells autophagy to mediate AR after LT, providing a theoretical basis for finding new drug targets for the prevention and treatment of AR after LT.

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