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Architecture of TAF11/TAF13/TBP complex suggests novel regulation properties of general transcription factor TFIID

机译:TAF11 / TAF13 / TBP复合物的体系结构表明一般转录因子TFIDD的新型调节特性

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摘要

General transcription factor TFIID is a key component of RNA polymerase II transcription initiation. Human TFIID is a megadalton-sized complex comprising TATA-binding protein (TBP) and 13 TBP-associated factors (TAFs). TBP binds to core promoter DNA, recognizing the TATA-box. We identified a ternary complex formed by TBP and the histone fold (HF) domain-containing TFIID subunits TAF11 and TAF13. We demonstrate that TAF11/TAF13 competes for TBP binding with TATA-box DNA, and also with the N-terminal domain of TAF1 previously implicated in TATA-box mimicry. In an integrative approach combining crystal coordinates, biochemical analyses and data from cross-linking mass-spectrometry (CLMS), we determine the architecture of the TAF11/TAF13/TBP complex, revealing TAF11/TAF13 interaction with the DNA binding surface of TBP. We identify a highly conserved C-terminal TBP-interaction domain (CTID) in TAF13, which is essential for supporting cell growth. Our results thus have implications for cellular TFIID assembly and suggest a novel regulatory state for TFIID function.
机译:通用转录因子TFIID是RNA聚合酶II转录起始的关键组成部分。人TFIID是一个兆吨级的复合物,包含TATA结合蛋白(TBP)和13种TBP相关因子(TAF)。 TBP与核心启动子DNA结合,识别出TATA-box。我们鉴定出由TBP和含组蛋白折叠(HF)域的TFIID亚基TAF11和TAF13形成的三元复合物。我们证明,TAF11 / TAF13与TATA盒DNA竞争TBP结合,也与TAF1盒拟态先前牵涉的TAF1的N末端域竞争。在结合晶体坐标,生化分析和交联质谱(CLMS)数据的整合方法中,我们确定了TAF11 / TAF13 / TBP复合物的体系结构,揭示了TAF11 / TAF13与TBP DNA结合表面的相互作用。我们在TAF13中识别出高度保守的C端TBP相互作用域(CTID),这对于支持细胞生长至关重要。因此,我们的结果对细胞TFIID组装具有影响,并暗示了TFIID功能的新型调节状态。

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