Title of article
Common Motifs and Topological Effects in the Protein Folding Transition State
Author/Authors
Isaac A. Hubner، نويسنده , , Magnus Lindberg، نويسنده , , Ellinor Haglund، نويسنده , , Mikael Oliveberg، نويسنده , , Jeffrey Skolnick and Eugene I. Shakhnovich، نويسنده ,
Issue Information
روزنامه با شماره پیاپی سال 2006
Pages
11
From page
1075
To page
1085
Abstract
Through extensive experiment, simulation, and analysis of protein S6 (1RIS), we find that variations in nucleation and folding pathway between circular permutations are determined principally by the restraints of topology and specific nucleation, and affected by changes in chain entropy. Simulations also relate topological features to experimentally measured stabilities. Despite many sizable changes in ϕ values and the structure of the transition state ensemble that result from permutation, we observe a common theme: the critical nucleus in each of the mutants share a subset of residues that can be mapped to the critical nucleus residues of the wild-type. Circular permutations create new N and C termini, which are the location of the largest disruption of the folding nucleus, leading to a decrease in both ϕ values and the role in nucleation. Mutant nuclei are built around the wild-type nucleus but are biased towards different parts of the S6 structure depending on the topological and entropic changes induced by the location of the new N and C termini.
Keywords
Ensemble , Simulation , circular permutant , protein S6 , Nucleation
Journal title
Journal of Molecular Biology
Serial Year
2006
Journal title
Journal of Molecular Biology
Record number
1248060
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