| Literature DB >> 31511645 |
Jing Guo1,2, Zhonghui Xue1,2, Ruoyu Ma1,2, Weiwei Yi3, Zhaoyuan Hui1,2, Yixin Guo1,2, Yuxi Yao1,2, Wenqiang Cao1,2, Jianli Wang1,2, Zhenyu Ju4, Linrong Lu5, Lie Wang6,7,8.
Abstract
The expression of coinhibitory receptors, such as CTLA-4, on effector T cells is a key mechanism for the negative regulation of T-cell activation. However, the transcriptional regulation of CTLA-4 is not well understood. Zfp281, a C2H2 zinc finger protein, is a negative regulator of pluripotency maintenance of embryonic stem cells. Nevertheless, the function of Zfp281 in differentiated cells has not been studied. We generated Zfp281 conditional knockout mice in which the function of the Zfp281 gene was conditionally disrupted by the Cd4Cre transgene to study its impact on T cell function. Zfp281 had no effect on T-cell development, but CD4+ T cell activation and cytokine production were impaired due to diminished T-cell receptor signaling. Furthermore, Zfp281 deficiency inhibited in vivo T cell responses to Listeria monocytogenes infection. Using genome-wide expression profiling assays, we determined that Zfp281 repressed Ctla-4 expression by directly binding to GC-rich sites in its promoter, which inhibited the negative feedback of T cell activation. In line with this result, CTLA-4 blockade and shRNA knockdown partly rescued the reduced cytokine production caused by Zfp281 deficiency. These findings indicate that Zfp281 sustains CD4+ T lymphocyte activation by directly repressing Ctla-4 transcription.Entities:
Keywords: CTLA-4; T cell activation; TCR signaling; Zfp281
Year: 2019 PMID: 31511645 PMCID: PMC7784856 DOI: 10.1038/s41423-019-0289-y
Source DB: PubMed Journal: Cell Mol Immunol ISSN: 1672-7681 Impact factor: 11.530