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由活化T细胞核因子介导的转录在效应性CD4 +辅助性T细胞2(Th2)中具有高度诱导性,而在Th1细胞中则不然。

Transcription mediated by NFAT is highly inducible in effector CD4+ T helper 2 (Th2) cells but not in Th1 cells.

作者信息

Rincón M, Flavell R A

机构信息

Section of Immunobiology, Yale University School of Medicine, New Haven, Connecticut 06510, USA.

出版信息

Mol Cell Biol. 1997 Mar;17(3):1522-34. doi: 10.1128/MCB.17.3.1522.

Abstract

Transcriptional factors of the NFAT family play an important role in regulating the expression of several cytokine genes during the immune response, such as the genes for interleukin 2 (IL-2) and IL-4, among others. Upon antigen stimulation, precursor CD4+ T helper (pTh) cells proliferate and differentiate into two populations of effector cells (eTh1 and eTh2), each one expressing a specific pattern of cytokines that distinguishes them from their precursors. eTh2 cells are the major source of IL-4, while gamma interferon is produced by eTh1 cells. Here we have used reporter transgenic mice to show that DNA binding and transcriptional activities of NFAT are transiently induced during the differentiation of pTh cells into either eTh1 or eTh2 cells to mediate the expression of IL-2 as a common growth factor in both pathways. However, although NFAT DNA binding is similarly induced in both eTh1 and eTh2 cells upon antigen stimulation, only the NFAT complexes present in eTh2 cells are able to mediate high-level transcription, and relatively little NFAT transcriptional activity was induced in eTh1 cells. In contrast to activated pTh cells, neither eTh1 nor eTh2 cells produced significant IL-2 upon stimulation, but the high levels of NFAT transcriptional activities directly correlate with the IL-4 production induced in response to antigen stimulation in eTh2 cells. These data suggest that activated NFAT is involved in the effector function of eTh2 cells and that the failure of eTh1 cells to produce IL-4 in response to an antigen is due, at least partially, to a failure to induce high-level transcription of the IL-4 gene by NFAT. Regulation of NFAT could be therefore a critical element in the polarization to eTh1 or eTh2.

摘要

NFAT家族的转录因子在免疫反应过程中对多种细胞因子基因的表达调控起着重要作用,比如白细胞介素2(IL-2)和IL-4等基因。在抗原刺激下,前体CD4 +辅助性T细胞(pTh)增殖并分化为两个效应细胞群体(eTh1和eTh2),每个群体表达特定的细胞因子模式,从而与它们的前体区分开来。eTh2细胞是IL-4的主要来源,而γ干扰素由eTh1细胞产生。在此,我们利用报告基因转基因小鼠表明,在pTh细胞分化为eTh1或eTh2细胞的过程中,NFAT的DNA结合和转录活性会被短暂诱导,以介导IL-2作为两种途径中共同生长因子的表达。然而,尽管抗原刺激后eTh1和eTh2细胞中NFAT的DNA结合被类似地诱导,但只有eTh2细胞中存在的NFAT复合物能够介导高水平转录,而eTh1细胞中诱导的NFAT转录活性相对较低。与活化的pTh细胞不同,eTh1和eTh2细胞在刺激后均不产生显著的IL-2,但高水平的NFAT转录活性与eTh2细胞中抗原刺激诱导的IL-4产生直接相关。这些数据表明,活化的NFAT参与eTh2细胞的效应功能,并且eTh1细胞在抗原刺激下不能产生IL-4至少部分是由于NFAT未能诱导IL-4基因的高水平转录。因此,NFAT的调控可能是向eTh1或eTh2极化的关键因素。

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