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Rewiring mitochondrial metabolism to counteract exhaustion of CAR-T cells.

Yue HuangXiaohui SiMi ShaoXinyi TengGang XiaoHe Huang
Published in: Journal of hematology & oncology (2022)
Short persistence and early exhaustion of T cells are major limits to the efficacy and broad application of immunotherapy. Exhausted T and chimeric antigen receptor (CAR)-T cells upregulate expression of genes associated with terminated T cell differentiation, aerobic glycolysis and apoptosis. Among cell exhaustion characteristics, impaired mitochondrial function and dynamics are considered hallmarks. Here, we review the mitochondrial characteristics of exhausted T cells and particularly discuss different aspects of mitochondrial metabolism and plasticity. Furthermore, we propose a novel strategy of rewiring mitochondrial metabolism to emancipate T cells from exhaustion and of targeting mitochondrial plasticity to boost CAR-T cell therapy efficacy.
Keyphrases
  • oxidative stress
  • cell therapy
  • stem cells
  • single cell
  • cell proliferation
  • drug delivery
  • signaling pathway
  • pi k akt