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机制守恒,速率变化:三种同源四螺旋束蛋白的折叠动力学

Conservation of mechanism, variation of rate: folding kinetics of three homologous four-helix bundle proteins.

作者信息

Dalal Seema, Canet Denis, Kaiser Stephen E, Dobson Christopher M, Regan Lynne

机构信息

Department of Chemistry, Yale University, New Haven, CT 06520-8114, USA.

出版信息

Protein Eng Des Sel. 2008 Mar;21(3):197-206. doi: 10.1093/protein/gzm088.

Abstract

The amino acid sequence of a protein determines both its final folded structure and the folding mechanism by which this structure is attained. The differences in folding behaviour between homologous proteins provide direct insights into the factors that influence both thermodynamic and kinetic properties. Here, we present a comprehensive thermodynamic and kinetic analysis of three homologous homodimeric four-helix bundle proteins. Previous studies with one member of this family, Rop, revealed that both its folding and unfolding behaviour were interesting and unusual: Rop folds (k(0)(f) = 29 s(-1)) and unfolds (k(0)(u) = 6 x 10(-7) s(-1)) extremely slowly for a protein of its size that contains neither prolines nor disulphides in its folded structure. The homologues we discuss have significantly different stabilities and rates of folding and unfolding. However, the rate of protein folding directly correlates with stability for these homologous proteins: proteins with higher stability fold faster. Moreover, in spite of possessing differing thermodynamic and kinetic properties, the proteins all share a similar folding and unfolding mechanism. We discuss the properties of these naturally occurring Rop homologues in relation to previously characterized designed variants of Rop.

摘要

蛋白质的氨基酸序列决定了其最终的折叠结构以及获得该结构的折叠机制。同源蛋白质之间折叠行为的差异为影响热力学和动力学性质的因素提供了直接的见解。在这里,我们对三种同源同二聚体四螺旋束蛋白进行了全面的热力学和动力学分析。此前对该家族的一个成员Rop的研究表明,其折叠和去折叠行为既有趣又不寻常:对于其大小且折叠结构中既不含脯氨酸也不含二硫键的蛋白质来说,Rop折叠(k(0)(f) = 29 s(-1))和去折叠(k(0)(u) = 6×10(-7) s(-1))极其缓慢。我们所讨论的同源物具有显著不同的稳定性以及折叠和去折叠速率。然而,对于这些同源蛋白质而言,蛋白质折叠速率与稳定性直接相关:稳定性较高的蛋白质折叠得更快。此外,尽管这些蛋白质具有不同的热力学和动力学性质,但它们都共享相似的折叠和去折叠机制。我们将这些天然存在的Rop同源物的性质与先前表征的Rop设计变体进行了讨论。

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