小单结构域蛋白折叠的结构见解。

The Italian journal of biochemistry Pub Date : 2003-12-01
Stefano Gianni, Ugo Mayor, Alan R Fersht
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引用次数: 0

摘要

了解多肽链折叠成其独特的天然结构的机制需要对折叠过程中所有物种的结构和动态特性进行完整和详细的描述。在小的单结构域蛋白质的情况下,实验研究正在以接近原子的分辨率定义变性态、折叠中间体和过渡态的结构。此外,理论家和实验家之间的协同作用现在允许对整个(非)折叠途径的详细描述。在这里,我们讨论了从这些研究中开始出现的变性态、折叠中间体和过渡态的一些一般结构方面。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Structural insights in the folding of small single-domain proteins.

Understanding the mechanism by which a polypeptide chain folds into its unique native structure requires a complete and detailed description of the structural and dynamic properties of all the species populated in the folding process. In the case of small single domain proteins, experimental studies are defining the structures of denatured states, folding intermediates and transition states at nearly atomic resolution. Further, the synergy between theoreticians and experimentalists is now allowing the detailed description of whole (un)folding pathways. Here, we discuss some of the general structural aspects of the denatured states, folding intermediates and transition states that are beginning to emerge from these studies.

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