European Journal of Medical Research (Dec 2024)

Tim-3 pathway dysregulation and targeting in sepsis-induced immunosuppression

  • Jialiu Luo,
  • Cong Zhang,
  • Deng Chen,
  • Teding Chang,
  • Shunyao Chen,
  • Zhiqiang Lin,
  • Chengla Yi,
  • Zhao-Hui Tang

DOI
https://doi.org/10.1186/s40001-024-02203-w
Journal volume & issue
Vol. 29, no. 1
pp. 1 – 13

Abstract

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Abstract Sepsis is a major medical problem which causes millions of deaths worldwide every year. The host immune response in sepsis is characterized by acute inflammation and a simultaneous state of immunosuppression. In the later stage of sepsis, immunosuppression is a crucial factor that increases the susceptibility of septic patients to secondary infection and mortality. It is characterized by T cell exhaustion, excessive production of anti-inflammatory cytokines, hyperproliferation of immune suppressor cells and aberrant expression of immune checkpoint molecules. T cell immunoglobulin and mucin domain 3 (Tim-3), an immune checkpoint molecule, is found on the surface of various cells, including macrophages, NK cells, NKT cells, and T cells. There are four different ligands for Tim-3, and accumulating evidence indicates that Tim-3 and its ligands play a crucial role in regulating immune cell dysfunction during sepsis. Anti-Tim-3 antibodies have been applied in the field of cancer immunotherapy and have achieved positive therapeutic effects in some clinical trials. However, the therapeutic efficacy of Tim-3 blockade is still controversial in animal models of sepsis. These challenges highlight the need for a deeper understanding of Tim-3 signaling in sepsis. This review examines the comprehensive effect of Tim-3 signaling in the development of sepsis-induced immunosuppression and the therapeutic efficacy of Tim-3 blockade.

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