RNA 聚合酶 II C 端七肽重复结构域丝氨酸 7 位磷酸化是在中介体依赖性方式下建立的。
RNA polymerase II C-terminal heptarepeat domain Ser-7 phosphorylation is established in a mediator-dependent fashion.
机构信息
Institute of Molecular Tumor Biology, University of Muenster, Robert-Koch-Strasse 43, 48149 Muenster, Germany.
出版信息
J Biol Chem. 2010 Jan 1;285(1):188-96. doi: 10.1074/jbc.M109.046565. Epub 2009 Nov 9.
Abstract
The largest subunit of RNA polymerase II (RNAPII) C-terminal heptarepeat domain (CTD) is subject to phosphorylation during initiation and elongation of transcription by RNA polymerase II. Here we study the molecular mechanisms leading to phosphorylation of Ser-7 in the human enzyme. Ser-7 becomes phosphorylated before initiation of transcription at promoter regions. We identify cyclin-dependent kinase 7 (CDK7) as one responsible kinase. Phosphorylation of both Ser-5 and Ser-7 is fully dependent on the cofactor complex Mediator. A subform of Mediator associated with an active RNAPII is critical for preinitiation complex formation and CTD phosphorylation. The Mediator-RNAPII complex independently recruits TFIIB and CDK7 to core promoter regions. CDK7 phosphorylates Ser-7 selectively in the context of an intact preinitiation complex. CDK7 is not the only kinase that can modify Ser-7 of the CTD. ChIP experiments with chemical inhibitors provide evidence that other yet to be identified kinases further phosphorylate Ser-7 in coding regions.
摘要
RNA 聚合酶 II(RNAPII)最大亚基 C 端七肽重复结构域(CTD)在 RNA 聚合酶 II 起始和延伸转录过程中会发生磷酸化。本文研究了导致人源酶 Ser-7 磷酸化的分子机制。Ser-7 在启动子区域的转录起始之前发生磷酸化。我们发现细胞周期蛋白依赖性激酶 7(CDK7)是一个负责磷酸化的激酶。Ser-5 和 Ser-7 的磷酸化完全依赖于中介复合物。与活性 RNAPII 相关的中介体亚基对于起始前复合物的形成和 CTD 磷酸化至关重要。中介体-RNAPII 复合物可独立招募 TFIIB 和 CDK7 至核心启动子区域。在完整的起始前复合物中,CDK7 选择性地磷酸化 Ser-7。CDK7 并不是唯一可以修饰 CTD Ser-7 的激酶。用化学抑制剂进行 ChIP 实验提供了证据,表明其他尚未鉴定的激酶在编码区进一步磷酸化 Ser-7。
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