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The structure of the transition state for the association of two fragments of the barley chymotrypsin inhibitor 2 to generate native-like protein: implications for mechanisms of protein folding.

机译:大麦胰凝乳蛋白酶抑制剂2的两个片段缔合以生成天然蛋白的过渡态结构:对蛋白质折叠机制的影响。

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摘要

Possible early events in protein folding may be studied by dissecting proteins into complementary fragments. Two fragments of chymotrypsin inhibitor 2 [CI2-(20-59) and CI2-(60-83)] associate to form a native-like structure in a second-order reaction that combines collision and rearrangement. The transition state of the reaction, analyzed by the protein engineering method on 17 mutants, is remarkably similar to that for the folding of the intact protein--a structure that resembles an expanded version of the folded structure with most interactions significantly weakened. The exception is that the N-terminal region of the single alpha-helix (the N-capping box) is completely formed in the transition state for association of the fragments, whereas it is reasonably well formed for the intact protein. Preliminary evidence on the structures of the individual fragments indicates that both are mainly nonnative, lacking native secondary structure and having regions of nonnative buried hydrophobic clusters. The association reaction does not result from the collision of a subpopulation of two fully native-like fragments but involves a considerable rearrangement of structure.
机译:蛋白质折叠中可能的早期事件可通过将蛋白质切成互补片段来研究。胰凝乳蛋白酶抑制剂2的两个片段[CI2-(20-59)和CI2-(60-83)]在结合了碰撞和重排的二阶反应中结合形成天然结构。通过蛋白质工程方法对17个突变体进行分析,反应的过渡状态与完整蛋白质的折叠状态非常相似-这种结构类似于折叠结构的扩展形式,但大多数相互作用都被弱化了。唯一的例外是单个α螺旋的N末端区域(N帽盒)在过渡状态下完全形成,用于片段结合,而对于完整蛋白则形成得相当好。关于单个片段的结构的初步证据表明,两者均主要是非天然的,缺乏天然的二级结构,并且具有非天然的埋藏疏水性簇的区域。缔合反应不是由于两个完全天然的片段的亚群的碰撞而引起的,而是涉及相当大的结构重排。

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