The Kinase Complex mTOR Complex 2 Promotes the Follicular Migration and Functional Maturation of Differentiated Follicular Helper CD4+ T Cells During Viral Infection

激酶复合物 mTOR 复合物 2 在病毒感染期间促进分化滤泡辅助性 CD4+ T 细胞的滤泡迁移和功能成熟

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作者:Yaxing Hao ,Yifei Wang ,Xiaobing Liu ,Xia Yang ,Pengcheng Wang ,Qin Tian ,Qiang Bai ,Xiangyu Chen ,Zhirong Li ,Jialin Wu ,Zhunyi Xie ,Xinyuan Zhou ,Yuyang Zhou ,Zhinan Yin ,Yuzhang Wu ,Lilin Ye

Abstract

Follicular helper CD4+ T (TFH) cells are critical for optimal B-cell-mediated humoral immunity by initiating, fueling, and sustaining germinal center reactions. The differentiation of TFH cells relies on multiple intrinsic and extrinsic factors; however, the details by which these factors are integrated to coordinate TFH differentiation are largely unknown. In this study, using a mouse model of acute lymphocytic choriomeningitis virus (LCMV) viral infection, we demonstrate that mTOR complex 2 (mTORC2) kinase integrates TCR signaling and ICOS-mediated co-stimulation to promote late differentiation and functional maturation of virus-specific TFH cells. Specifically, mTORC2 functions to maintain TFH lineage specifications, including phenotypes, migratory characteristics, and functional properties. Thus, our results highlight the importance of mTORC2 in guarding TFH phenotypic and functional maturation.

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