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Characterization of RNA helicase A as component of STAT6-dependent enhanceosome

机译:RNA解旋酶A作为STAT6依赖性增强体成分的表征

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Signal transducer and activator of transcription 6 (STAT6) is a regulator of transcription for interleukin-4 (IL-4)-induced genes. The ability of STAT6 to activate transcription depends on functional interaction with other transcription factors and coactivators. We have characterized the mechanism of STAT6-mediated transcriptional activation by identifying STAT6 transcription activation domain (TAD) interacting nuclear proteins. The first of the identified proteins was coactivator protein p100, which regulates IL-4-induced transcription by connecting STAT6 with other transcriptional regulators. Here, we describe RNA helicase A (RHA) as a novel component of STAT6 transcriptosome. In vitro and in vivo experiments indicated that RHA did not directly interact with STAT6, but p100 protein was found to mediate the assembly of the ternary complex of STAT6-p100-RHA. In chromatin immuno-precipitation studies RHA together with p100 enhanced the binding of STAT6 on the human Ig epsilon promoter after IL-4 stimulation. RHA enhanced the IL-4-induced transcription, and the participation of RHA in IL-4-regulated transcription was supported by RNAi experiments. Our results suggest that RHA has an important role in the assembly of STAT6 transcriptosome. As RHA is also known to interact with chromatin modifying proteins, the RHA containing protein complexes may facilitate the entry of transcriptional apparatus to the IL-4 responsive promoters.
机译:信号转导和转录激活因子6(STAT6)是白介素4(IL-4)诱导的基因的转录调节因子。 STAT6激活转录的能力取决于与其他转录因子和共激活因子的功能相互作用。我们通过鉴定STAT6转录激活域(TAD)相互作用的核蛋白来表征STAT6介导的转录激活的机制。鉴定出的第一个蛋白是共激活蛋白p100,它通过将STAT6与其他转录调节因子连接来调节IL-4诱导的转录。在这里,我们描述RNA解旋酶A(RHA)作为STAT6转录体的新型成分。体外和体内实验表明,RHA不与STAT6直接相互作用,但发现p100蛋白介导STAT6-p100-RHA三元复合物的装配。在染色质免疫沉淀研究中,RHA与p100一起增强了IL-4刺激后STAT6在人Igε启动子上的结合。 RHA增强了IL-4诱导的转录,RNAi实验支持RHA参与IL-4调控的转录。我们的结果表明,RHA在STAT6转录体的组装中具有重要作用。由于还已知RHA与染色质修饰蛋白发生相互作用,因此包含RHA的蛋白复合物可促进转录装置进入IL-4响应性启动子。

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