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Bioinformatical parsing of folding-on-binding proteins reveals their compositional and evolutionary sequence design

机译:结合蛋白折叠的生物信息学分析揭示了它们的组成和进化序列设计

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摘要

Intrinsic disorder occurs when (part of) a protein remains unfolded during normal functioning. Intrinsically-disordered regions can contain segments that ‘fold on binding’ to another molecule. Here, we perform bioinformatical parsing of human ‘folding-on-binding’ (FB) proteins, into four subsets: Ordered regions, FB regions, Disordered regions that surround FB regions (‘Disordered-around-FB’), and Other-Disordered regions. We examined the composition and evolutionary behaviour (across vertebrate orthologs) of these subsets. From a convergence of three separate analyses, we find that for hydrophobicity, Ordered regions segregate from the other subsets, but the Ordered and FB regions group together as highly conserved, and the Disordered-around-FB and Other-Disordered regions as less conserved (with a lesser significant difference between Ordered and FB regions). FB regions are highly-conserved with net positive charge, whereas Disordered-around-FB have net negative charge and are relatively less hydrophobic than FB regions. Indeed, these Disordered-around-FB regions are excessively hydrophilic compared to other disordered regions generally. We describe how our results point towards a possible compositionally-based steering mechanism of folding-on-binding.
机译:当蛋白质(的一部分)在正常功能过程中仍未折叠时,就会发生内源性疾病。本质上无序的区域可能包含与另一分子“结合时折叠”的片段。在这里,我们将人的“结合折叠”(FB)蛋白进行生物信息学解析,分为四个子集:有序区域,FB区,围绕FB区的无序区(“ Disordered-around-FB”)和“ Other-Disordered”地区。我们检查了这些子集的组成和进化行为(跨脊椎动物直系同源基因)。通过三个独立分析的收敛,我们发现对于疏水性而言,有序区域与其他子集隔离开来,但有序区域和FB区域分组为高度保守,而无序围绕FB和其他无序区域则较不保守(且有序区域和FB区域之间的差异较小)。 FB区的净正电荷高度保守,而Disordered-around-FB则具有净负电荷,且疏水性比FB区低。实际上,与其他无序区域相比,这些无序的FB区域亲水性过高。我们描述了我们的结果如何指向可能的基于装订折叠的基于操纵的操纵机制。

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