清脆的
生发中心
生物
细胞生物学
PI3K/AKT/mTOR通路
自噬
mTORC1型
信号转导
B细胞
免疫学
基因
抗体
遗传学
细胞凋亡
作者
Bruce Huang,James D. Phelan,Silvia Preite,Julio Gómez‐Rodriguez,Kjell Johansen,Hirofumi Shibata,Arthur L. Shaffer,Qunying Xu,Brendan M. Jeffrey,Martha Kirby,Stacie M. Anderson,Yandan Yang,Selamawit Gossa,Dorian B. McGavern,Louis M. Staudt,Pamela L. Schwartzberg
标识
DOI:10.1038/s41467-022-28378-6
摘要
T follicular helper (Tfh) cells provide signals to initiate and maintain the germinal center (GC) reaction and are crucial for the generation of robust, long-lived antibody responses, but how the GC microenvironment affects Tfh cells is not well understood. Here we develop an in vivo T cell-intrinsic CRISPR-knockout screen to evaluate Tfh and Th1 cells in an acute viral infection model to identify regulators of Tfh cells in their physiological setting. Using a screen of druggable-targets, alongside genetic, transcriptomic and cellular analyses, we identify a function of HIF-1α in suppressing mTORC1-mediated and Myc-related pathways, and provide evidence that VHL-mediated degradation of HIF-1α is required for Tfh development; an expanded in vivo CRISPR screen reveals multiple components of these pathways that regulate Tfh versus Th1 cells, including signaling molecules, cell-cycle regulators, nutrient transporters, metabolic enzymes and autophagy mediators. Collectively, our data serve as a resource for studying Tfh versus Th1 decisions, and implicate the VHL-HIF-1α axis in fine-tuning Tfh generation.
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