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Solution Structure of Tandem SH2 Domains from Spt6 Protein and Their Binding to the Phosphorylated RNA Polymerase II C-terminal Domain

机译:Spt6蛋白的串联SH2域的溶液结构及其与磷酸化RNA聚合酶II C末端域的结合

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摘要

Spt6 is a highly conserved transcription elongation factor and histone chaperone. It binds directly to the RNA polymerase II C-terminal domain (RNAPII CTD) through its C-terminal region that recognizes RNAPII CTD phosphorylation. In this study, we determined the solution structure of the C-terminal region of Saccharomyces cerevisiae Spt6, and we discovered that Spt6 has two SH2 domains in tandem. Structural and phylogenetic analysis revealed that the second SH2 domain was evolutionarily distant from canonical SH2 domains and represented a novel SH2 subfamily with a novel binding site for phosphoserine. In addition, NMR chemical shift perturbation experiments demonstrated that the tandem SH2 domains recognized Tyr1, Ser2, Ser5, and Ser7 phosphorylation of RNAPII CTD with millimolar binding affinities. The structural basis for the binding of the tandem SH2 domains to different forms of phosphorylated RNAPII CTD and its physiological relevance are discussed. Our results also suggest that Spt6 may use the tandem SH2 domain module to sense the phosphorylation level of RNAPII CTD.
机译:Spt6是高度保守的转录延伸因子和组蛋白伴侣。它通过识别RNAPII CTD磷酸化的C端区域直接与RNA聚合酶II C端结构域(RNAPII CTD)结合。在这项研究中,我们确定了酿酒酵母Spt6 C末端区域的溶液结构,我们发现Spt6具有两个串联的SH2域。结构和系统发育分析表明,第二个SH2结构域与经典的SH2结构域在进化上相距甚远,代表了一个新的SH2亚家族,具有一个新的磷酸丝氨酸结合位点。此外,NMR化学位移扰动实验表明串联的SH2域识别Tyr 1 ,Ser 2 ,Ser 5 和Ser RNAPII CTD的7 磷酸化,具有毫摩尔结合亲和力。讨论了串联SH2结构域与不同形式的磷酸化RNAPII CTD结合的结构基础及其生理相关性。我们的结果还表明,Spt6可能使用串联SH2域模块来检测RNAPII CTD的磷酸化水平。

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