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首页> 外文期刊>Immunity >Discrete roles of STAT4 and STAT6 transcription factors in tuning epigenetic modifications and transcription during T helper cell differentiation.
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Discrete roles of STAT4 and STAT6 transcription factors in tuning epigenetic modifications and transcription during T helper cell differentiation.

机译:STAT4和STAT6转录因子在调节T辅助细胞分化过程中表观遗传修饰和转录中的离散作用。

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摘要

Signal transducer and activator of transcription 4 (STAT4) and STAT6 are key factors in the specification of helper T cells; however, their direct roles in driving differentiation are not well understood. Using chromatin immunoprecipitation and massive parallel sequencing, we quantitated the full complement of STAT-bound genes, concurrently assessing global STAT-dependent epigenetic modifications and gene transcription by using cells from cognate STAT-deficient mice. STAT4 and STAT6 each bound over 4000 genes with distinct binding motifs. Both played critical roles in maintaining chromatin configuration and transcription of a core subset of genes through the combination of different epigenetic patterns. Globally, STAT4 had a more dominant role in promoting active epigenetic marks, whereas STAT6 had a more prominent role in antagonizing repressive marks. Clusters of genes negatively regulated by STATs were also identified, highlighting previously unappreciated repressive roles of STATs. Therefore, STAT4 and STAT6 play wide regulatory roles in T helper cell specification.
机译:信号转导子和转录激活子4(STAT4)和STAT6是辅助T细胞规格的关键因素。然而,人们对它们在促进差异化方面的直接作用还知之甚少。使用染色质免疫沉淀和大规模并行测序,我们定量了STAT结合基因的完整互补,同时通过使用同源STAT缺陷小鼠的细胞,同时评估了全球STAT依赖的表观遗传修饰和基因转录。 STAT4和STAT6各自结合了4000多个具有不同结合基序的基因。两者在通过不同表观遗传模式的组合来维持染色质构型和基因核心子集的转录中起着关键作用。在全球范围内,STAT4在促进活动表观遗传标记方面具有更主要的作用,而STAT6在拮抗抑制性标记方面具有更突出的作用。还鉴定了由STATs负调控的基因簇,突显了STATs以前没有意识到的抑制作用。因此,STAT4和STAT6在T辅助细胞规范中起着广泛的调节作用。

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