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首页> 外文期刊>Molecular cancer research: MCR >Crystal structure of a multidomain human p53 tetramer bound to the natural CDKN1A (p21) p53-response element.
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Crystal structure of a multidomain human p53 tetramer bound to the natural CDKN1A (p21) p53-response element.

机译:多域人类p53四聚体的晶体结构与天然CDKN1A(p21)p53反应元件结合。

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摘要

The p53 tumor suppressor protein is a sequence-specific DNA-binding transcription factor. Structures of p53 bound to DNA have been described, but, so far, no structure has been determined of p53 bound to a natural p53-response element. We describe here the structure of a human p53 homotetramer encompassing both the DNA-binding and homo-oligomerization domains in complex with the natural p53-response element present upstream of the promoter of the CDKN1A (p21) gene. Similar to our previously described structures of human p53 tetramers bound to an artificial consensus DNA site, p53 DNA binding proceeds via an induced fit mechanism with loops L1 of two subunits adopting recessed conformations. Interestingly, the conformational change involving loop L1 is even more extreme than the one previously observed with the artificial consensus DNA site. In fact, the previously determined loop L1 conformation seems to be a transition intermediate between the non-DNA-bound and CDKN1A-bound states. Thus, the new structure further supports our model that recognition of specific DNA by p53 is associated with conformational changes within the DNA-binding domain of p53.
机译:p53肿瘤抑制蛋白是一种序列特异性的DNA结合转录因子。已经描述了与DNA结合的p53的结构,但是到目前为止,还没有确定与天然p53反应元件结合的p53的结构。我们在这里描述了人类p53同四聚体的结构,该结构包含与CDKN1A(p21)基因启动子上游存在的天然p53反应元件复合的DNA结合和同聚域。类似于我们先前描述的人p53四聚体与人工共有DNA位点结合的结构,p53 DNA结合通过诱导的嵌合机制进行,其中两个亚基的环L1采用凹陷构象。有趣的是,涉及环L1的构象变化甚至比以前在人工共有DNA位点上观察到的更为极端。实际上,先前确定的环L1构象似乎是非DNA结合状态与CDKN1A结合状态之间的过渡中间位。因此,新结构进一步支持了我们的模型,即p53对特定DNA的识别与p53的DNA结合域内的构象变化有关。

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