B7-H3 confers resistance to Vγ9Vδ2 T cell-mediated cytotoxicity in human colon cancer cells via the STAT3/ULBP2 axis.
Huimin LuYanchao MaMingyuan WangJin ShenHongya WuJuntao LiNan GaoYanzheng GuXueguang ZhangGuangbo ZhangTongguo ShiWeichang ChenPublished in: Cancer immunology, immunotherapy : CII (2020)
Immunotherapy based on γδT cells has limited efficiency in solid tumors, including colon cancer (CC). The immune evasion of tumor cells may be the main cause of the difficulties of γδT cell-based treatment. In the present study, we explored whether and how B7-H3 regulates the resistance of CC cells to the cytotoxicity of Vγ9Vδ2 (Vδ2) T cells. We observed that B7-H3 overexpression promoted, while B7-H3 knockdown inhibited, CC cell resistance to the killing effect of Vδ2 T cells in vitro and in vivo. Mechanistically, we showed that B7-H3-mediated CC cell resistance to the cytotoxicity of Vδ2 T cells involved a molecular pathway comprising STAT3 activation and decreased ULBP2 expression. ULBP2 blockade or knockdown abolished the B7-H3 silencing-induced increase in the cytotoxicity of Vδ2 T cells to CC cells. Furthermore, cryptotanshinone, a STAT3 phosphorylation inhibitor, reversed the B7-H3 overexpression-induced decrease in ULBP2 expression and attenuated the killing effect of Vδ2 T cells on CC cells. Moreover, there was a negative correlation between the expression of B7-H3 and ULBP2 in the tumor tissues of CC patients. Our results suggest that the B7-H3-mediated STAT3/ULBP2 axis may be a potential candidate target for improving the efficiency of γδT cell-based immunotherapy in CC.
Keyphrases
- induced apoptosis
- cell proliferation
- poor prognosis
- cell cycle arrest
- endothelial cells
- end stage renal disease
- gene expression
- endoplasmic reticulum stress
- newly diagnosed
- transcription factor
- ejection fraction
- binding protein
- cell therapy
- peritoneal dialysis
- climate change
- mesenchymal stem cells
- prognostic factors
- bone marrow
- replacement therapy