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首页> 外文期刊>Journal of Molecular Biology >Crystal structure of the lambda repressor C-terminal domain octamer.
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Crystal structure of the lambda repressor C-terminal domain octamer.

机译:λ阻遏物C端结构域八聚体的晶体结构。

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摘要

The three-dimensional structure of the lambda repressor C-terminal domain (CTD) has been determined at atomic resolution. In the crystal, the CTD forms a 2-fold symmetric tetramer that mediates cooperative binding of two repressor dimers to pairs of operator sites. Based upon this structure, a model was proposed for the structure of an octameric repressor that forms both in the presence and absence of DNA. Here, we have determined the structure of the lambda repressor CTD in three new crystal forms, under a wide variety of conditions. All crystals have essentially the same tetramer, confirming the results of the earlier study. One crystal form has two tetramers bound to form an octamer, which has the same overall architecture as the previously proposed model. An unexpected feature of the octamer in the crystal structure is a unique interaction at the tetramer-tetramer interface, formed by residues Gln209, Tyr210 and Pro211, which contact symmetry-equivalent residues from other subunits of the octamer. Interestingly, these residues are also located at the dimer-dimer interface, where the specific interactions are different. The structures thus indicate specific amino acid residues that, at least in principle, when altered could result in repressors that form tetramers but not octamers. Copyright 2001 Academic Press.
机译:λ阻遏物C末端域(CTD)的三维结构已在原子分辨率下确定。在晶体中,CTD形成2倍对称四聚体,介导两个阻遏物二聚体与操作位点对的协同结合。基于这种结构,提出了一种在DNA存在和不存在时均形成的八聚体阻遏物的结构模型。在这里,我们在多种条件下确定了三种新的晶体形式的λ阻遏物CTD的结构。所有晶体都具有基本相同的四聚体,证实了早期研究的结果。一种晶型具有两个四聚体,它们结合形成一个八聚体,其整体结构与先前提出的模型相同。八聚体在晶体结构中的一个出乎意料的特征是在四聚体-四聚体界面上的独特相互作用,该残基由残基Gln209,Tyr210和Pro211形成,它们与来自八聚体的其他亚基的对称等效残基接触。有趣的是,这些残基也位于二聚体-二聚体界面处,其中特定的相互作用是不同的。因此,结构指示特定的氨基酸残基,至少在原则上,当改变时,这些残基可导致形成四聚体而不形成八聚体的阻遏物。版权所有2001学术出版社。

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