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首页> 外文期刊>Biophysical Journal >Allosteric response is both conserved and variable across three CheY orthologs.
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Allosteric response is both conserved and variable across three CheY orthologs.

机译:在三个CheY直系同源物中,变构反应既保守又可变。

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摘要

A computational method to identify residues likely to initiate allosteric signals has been developed. The method is based on differences within stability and flexibility profiles between wild-type and perturbed structures as computed by a distance constraint model. Application of the approach to three bacterial chemotaxis protein Y (CheY) orthologs provides a comparison of allosteric response across protein family divergence. Interestingly, we observe a rich mixture of both conservation and variability within the identified allosteric sites. While similarity within the overall response parallels the evolutionary relationships, >50% of the best scoring putative sites are only identified in a single ortholog. These results suggest that detailed descriptions of intraprotein communication are substantially more variable than structure and function, yet do maintain some evolutionary relationships. Finally, structural clusters of large response identify four allosteric hotspots, including the beta4/alpha4 loop known to be critical to relaying the CheY phosphorylation signal.
机译:已经开发了一种计算方法来鉴定可能引发变构信号的残基。该方法基于由距离约束模型计算出的野生型和受扰动结构在稳定性和柔韧性方面的差异。该方法对三种细菌趋化性蛋白Y(CheY)直系同源物的应用提供了跨蛋白质家族分歧的变构反应的比较。有趣的是,我们在确定的变构位点中观察到了保守性和变异性的丰富混合物。虽然总体响应中的相似性与进化关系平行,但仅在单个直系同源物中鉴定出超过50%的最佳评分推定位点。这些结果表明,蛋白内通讯的详细描述远比结构和功能多变,但确实保持了某些进化关系。最后,具有高响应性的结构簇可确定四个变构热点,包括已知对中继CheY磷酸化信号至关重要的beta4 / alpha4环。

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