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首页> 外文期刊>Cellular immunology >Bim-mediated apoptosis and PD-1/PD-L1 pathway impair reactivity of PD1(+)/CD127(-) HCV-specific CD8(+) cells targeting the virus in chronic hepatitis C virus infection.
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Bim-mediated apoptosis and PD-1/PD-L1 pathway impair reactivity of PD1(+)/CD127(-) HCV-specific CD8(+) cells targeting the virus in chronic hepatitis C virus infection.

机译:Bim介导的凋亡和PD-1 / PD-L1通路损害了针对慢性丙型肝炎病毒感染的PD1(+)/ CD127(-)HCV特异性CD8(+)细胞的反应性。

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摘要

PD-1 molecule promotes anergy and IL-7 receptor (CD127) induces an anti-apoptotic effect on T cells. Correlation between PD-1/CD127 phenotype and hepatitis C virus (HCV)-specific CD8(+) cell reactivity in resolved infection (RI) after treatment and persistent HCV-infection (PI) was analysed. Directly ex vivo, PD-1 and CD127 expression on HCV-specific CD8(+) cells displayed a positive and negative correlation, respectively with viraemia. Proliferation after stimulation on PD-1(-)/CD127(+) cells from RI cases was preserved, while it was impaired on PD-1(+)/CD127(-) cells from PI patients. PD1(+)/CD127(+) population was observed in PI, and these maintained expansion ability but they did not target the virus. Frequency of PI cases with HCV-specific CD8(+) cell proliferation increased after anti-PD-L1 and anti-apoptotic treatment. Bim expression on HCV-specific CD8(+) cells from PI patients was enhanced. In conclusion, during chronic HCV infection non-reactive HCV-specific CD8(+) cells targeting the virus are PD-1(+)/CD127(-)/Bim(+) and, blocking apoptosis and PD-1/PD-L1 pathway on them enhances in vitro reactivity.
机译:PD-1分子促进无反应,IL-7受体(CD127)诱导对T细胞的抗凋亡作用。分析PD-1 / CD127表型与丙型肝炎病毒(HCV)特异性CD8(+)细胞反应性与治疗后和持久性HCV感染(PI)后的感染(RI)的相关性。直接离体,HCV特异性CD8(+)细胞上的PD-1和CD127表达分别显示与病毒血症呈正相关和负相关。在RI患者的PD-1(-)/ CD127(-)细胞上刺激后的增殖得以保留,而在PI患者的PD-1(+)/ CD127(-)细胞上受到抑制。在PI中观察到PD1(+)/ CD127(+)种群,它们保持了扩展能力,但没有针对病毒。抗PD-L1和抗凋亡治疗后,HCV特异性CD8(+)细胞增殖的PI病例的频率增加。 PI患者的HCV特异性CD8(+)细胞上的Bim表达得到增强。总之,在慢性HCV感染过程中,针对该病毒的非反应性HCV特异性CD8(+)细胞为PD-1(+)/ CD127(-)/ Bim(+),并阻止凋亡和PD-1 / PD-L1它们上的信号通路增强了体外反应性。

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