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Structure of p53 binding to the BAX response element reveals DNA unwinding and compression to accommodate base-pair insertion

机译:p53与BAX反应元件结合的结构揭示DNA的解链和压缩以适应碱基对插入

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摘要

The p53 core domain binds to response elements (REs) that contain two continuous half-sites as a cooperative tetramer, but how p53 recognizes discontinuous REs is not well understood. Here we describe the crystal structure of the p53 core domain bound to a naturally occurring RE located at the promoter of the Bcl-2-associated X protein (BAX) gene, which contains a one base-pair insertion between the two half-sites. Surprisingly, p53 forms a tetramer on the BAX-RE that is nearly identical to what has been reported on other REs with a 0-bp spacer. Each p53 dimer of the tetramer binds in register to a half-site and maintains the same protein–DNA interactions as previously observed, and the two dimers retain all the protein–protein contacts without undergoing rotation or translation. To accommodate the additional base pair, the DNA is deformed and partially disordered around the spacer region, resulting in an apparent unwinding and compression, such that the interactions between the dimers are maintained. Furthermore, DNA deformation within the p53-bound BAX-RE is confirmed in solution by site-directed spin labeling measurements. Our results provide a structural insight into the mechanism by which p53 binds to discontinuous sites with one base-pair spacer.
机译:p53核心域绑定到包含两个连续的半位点作为协作四聚体的响应元件(RE),但是p53如何识别不连续的RE尚不清楚。在这里,我们描述了p53核心结构域的晶体结构,该结构与位于Bcl-2相关X蛋白(BAX)基因启动子上的天然RE结合,该基因在两个半位点之间包含一个碱基对插入。出乎意料的是,p53在BAX-RE上形成四聚体,几乎与其他带有0 bp间隔基的RE所报道的相同。四聚体的每个p53二聚体均与一个半位对齐并保持与先前观察到的相同的蛋白质-DNA相互作用,并且两个二聚体保留了所有蛋白质-蛋白质接触,而无需进行旋转或翻译。为了容纳另外的碱基对,DNA在间隔区周围变形并部分地无序,导致明显的展开和压缩,从而维持了二聚体之间的相互作用。此外,通过定点旋转标记测量可确定溶液中p53结合的BAX-RE中的DNA变形。我们的结果为p53通过一个碱基对间隔子结合到不连续位点的机理提供了结构上的见识。

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