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Protein folding and function: the N-terminal fragment in adenylate kinase.

机译:蛋白质折叠和功能:腺苷酸激酶的N末端片段。

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摘要

Three-dimensional protein folds range from simple to highly complex architectures. In complex folds, some building block fragments are more important for correct protein folding than others. Such fragments are typically buried in the protein core and mediate interactions between other fragments. Here we present an automated, surface area-based algorithm that is able to indicate which, among all local elements of the structure, is critical for the formation of the native fold, and apply it to structurally well-characterized proteins. In particular, we focus on adenylate kinase. The fragment containing the phosphate binding, P-loop (the "giant anion hole") flanked by a beta-strand and an alpha-helix near the N-terminus, is identified as a critical building block. This building block shows a high degree of sequence and structural conservation in all adenylate kinases. The results of our molecular dynamics simulations are consistent with this identification. In its absence, the protein flips to a stable, non-native state. In this misfolded conformation, the other local elements of the structure are in their native-like conformations; however, their association is non-native. Furthermore, this element is critically important for the function of the enzyme, coupling folding, and function.
机译:三维蛋白质折叠范围从简单到高度复杂的体系结构。在复杂的折叠中,对于正确的蛋白质折叠而言,某些构建基片段比其他片段更为重要。此类片段通常被埋在蛋白质核心中,并介导其他片段之间的相互作用。在这里,我们提出了一种基于表面积的自动化算法,该算法能够指出结构的所有局部元素中哪些对形成天然折叠至关重要,并将其应用于结构良好的蛋白质。特别地,我们专注于腺苷酸激酶。含有磷酸盐结合的P环(“巨大的阴离子孔”)的片段在N端附近有一个β链和一个α螺旋,被认为是关键的构建单元。该构件显示所有腺苷酸激酶中高度的序列和结构保守性。我们分子动力学模拟的结果与此鉴定相符。在缺乏蛋白质的情况下,蛋白质会转变为稳定的非天然状态。在这种错叠的构象中,结构的其他局部元素处于其天然样构象。但是,它们的关联是非本地的。此外,该元素对于酶的功能,偶联折叠和功能至关重要。

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