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NFAT 在 CD4+ T 辅助细胞效应功能中起着关键作用。

NFAT pulls the strings during CD4+ T helper cell effector functions.

机构信息

Department for Medical Genetics, Molecular and Clinical Pharmacology, Medical University Innsbruck, Innsbruck, Austria.

出版信息

Blood. 2010 Apr 15;115(15):2989-97. doi: 10.1182/blood-2009-10-233585. Epub 2010 Jan 26.

Abstract

The Ca(2+) dependent transcription factor family known as nuclear factor of activated T cells (NFAT) has been shown to be important in T-cell immune responses. Because NFAT proteins have a weak DNA-binding capacity, they cooperate with other transcription factors at composite sites within the promoters of target genes. Recently, NFAT was shown to also be important for the induction of specific genetic programs that guide the differentiation and effector or regulatory activities of CD4(+) T helper subsets via the transcriptional regulation of their lineage-specific transcription factors, specifically T-bet (Th1), Gata3 (Th2), RORgammat (Th17), and Foxp3 (iTregs). In addition, the NFAT family governs the transcription of several signature cytokines, including their cytokine receptors. Subsequently, the integration of these complex intracellular signal transduction cascades is considered to critically determine the crosstalk between the T-cell receptor and receptors that are activated by both the adaptive and innate immune systems to determine pathways of T helper cell differentiation and function. Here, we carefully review the critical role of the established transcriptional partners and functional outcomes of these NFAT interactions in regard to the effector responses of these clinically relevant CD4(+) T helper subsets.

摘要

已知钙依赖转录因子家族核因子活化 T 细胞(NFAT)在 T 细胞免疫反应中非常重要。由于 NFAT 蛋白与 DNA 的结合能力较弱,它们在靶基因启动子内的复合位点与其他转录因子合作。最近,NFAT 也被证明对于诱导特定的遗传程序很重要,这些程序通过其谱系特异性转录因子(T-bet[Th1]、Gata3[Th2]、RORgammat[Th17]和 Foxp3[iTregs])的转录调控,指导 CD4+T 辅助亚群的分化和效应或调节活性。此外,NFAT 家族调控包括其细胞因子受体在内的几种特征细胞因子的转录。随后,这些复杂的细胞内信号转导级联的整合被认为是决定 T 细胞受体与适应性和固有免疫系统激活的受体之间相互作用的关键,以确定 T 辅助细胞分化和功能的途径。在这里,我们仔细回顾了这些 NFAT 相互作用的既定转录伙伴和功能结果在这些临床相关 CD4+T 辅助亚群的效应反应中的关键作用。

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