KLF2 maintains lineage fidelity and suppresses CD8 T cell exhaustion during acute LCMV infection

IF 45.8 1区综合性期刊 Q1 MULTIDISCIPLINARY SCIENCES Science Pub Date : 2025-02-14

Eric Fagerberg, John Attanasio, Christine Dien, Jaiveer Singh, Emily A. Kessler, Leena Abdullah, Jian Shen, Brian G. Hunt, Kelli A. Connolly, Edward De Brouwer, Jiaming He, Nivedita R. Iyer, Jessica Buck, Emily R. Borr, Martina Damo, Gena G. Foster, Josephine R. Giles, Yina H. Huang, John S. Tsang, Smita Krishnaswamy, Weiguo Cui, Nikhil S. Joshi

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Abstract

Naïve CD8 T cells have the potential to differentiate into a spectrum of functional states during an immune response. How these developmental decisions are made and what mechanisms exist to suppress differentiation toward alternative fates remains unclear. We employed in vivo CRISPR-Cas9–based perturbation sequencing to assess the role of ~40 transcription factors (TFs) and epigenetic modulators in T cell fate decisions. Unexpectedly, we found that knockout of the TF Klf2 resulted in aberrant differentiation to exhausted-like CD8 T cells during acute infection. KLF2 was required to suppress the exhaustion-promoting TF TOX and to enable the TF TBET to drive effector differentiation. KLF2 was also necessary to maintain a polyfunctional tumor-specific progenitor state. Thus, KLF2 provides effector CD8 T cell lineage fidelity and suppresses the exhaustion program.

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在急性LCMV感染期间，KLF2维持谱系保真度并抑制CD8 T细胞衰竭

Naïve CD8 T细胞在免疫应答过程中具有分化成一系列功能状态的潜力。这些发展决定是如何做出的，以及存在什么机制来抑制向其他命运的分化，目前尚不清楚。我们使用基于crispr - cas9的体内微扰测序来评估约40个转录因子（tf）和表观遗传调节剂在T细胞命运决定中的作用。出乎意料的是，我们发现敲除TF Klf2导致急性感染期间异常分化为耗尽样CD8 T细胞。需要KLF2来抑制促筋疲力尽的TF TOX，并使TF TBET驱动效应因子分化。KLF2也是维持多功能肿瘤特异性祖细胞状态所必需的。因此，KLF2提供了效应CD8 T细胞谱系保真度并抑制了耗竭程序。

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来源期刊

Science 综合性期刊-综合性期刊

CiteScore

61.10

自引率

0.90%

发文量

审稿时长

2.1 months

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