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首页> 外文期刊>Journal of Molecular Biology >Discerning the structure and energy of multiple transition states in protein folding using psi-analysis.
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Discerning the structure and energy of multiple transition states in protein folding using psi-analysis.

机译:使用psi分析识别蛋白质折叠中多个过渡态的结构和能量。

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摘要

We quantify the degree to which folding occurs along a complex landscape with structurally distinct pathways using psi-analysis in combination with a protein engineering method that identifies native, non-covalent polypeptide interactions and their relative populations at the rate-limiting step. By probing the proximity of two specific partners, this method is extremely well-suited for comparison to theoretical simulations. Using ubiquitin as a model system, we detect individual pathways with site-resolved resolution, demonstrating that the protein folds through a native-like transition state ensemble with a common nucleus that contains heterogeneous features on its periphery. The consensus transition state topology has part of the major helix docked against four properly aligned beta-strands. However, structural heterogeneity exists in the transition state ensemble, wherein peripheral regions are differentially populated according to their relative stability. Pathway diversity reflects the variable order of formation of these peripheral elements, which radiate outward from the common nucleus. These results, which show only moderate agreement with traditional mutational phi-analysis, provide an extraordinarily detailed and quantitative description of protein folding.
机译:我们使用psi分析结合蛋白质工程方法来量化沿着复杂的景观以结构上不同的途径发生折叠的程度,该蛋白质工程方法可在限速步骤中识别天然的非共价多肽相互作用及其相对种群。通过探测两个特定伙伴的接近度,该方法非常适合与理论模拟进行比较。使用泛素作为模型系统,我们以位点分辨的分辨率检测单个途径,证明该蛋白折叠通过一个天然样的过渡态集合体,该集合体具有一个在外围包含异质性特征的共同核。共有过渡态拓扑的主要螺旋部分与四个正确排列的β链对接。但是,结构异质性存在于过渡状态集合中,其中外围区域根据其相对稳定性而差异地填充。途径的多样性反映了这些外围元素形成的可变顺序,这些外围元素从共同核向外辐射。这些结果仅显示与传统突变phi分析的适度一致,提供了蛋白质折叠的极其详细和定量的描述。

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