Non-native interactions play an effective role in protein folding dynamics.
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TL;DR: The results suggest that the stabilization of the folding transition state can be achieved through the establishment of a very small network of native contacts that are the first to lock during the folding process.
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Abstract: Systematic Monte Carlo simulations of simple lattice models show that the final stage of protein folding is an ordered process where native contacts get locked (i.e., the residues come into contact and remain in contact for the duration of the folding process) in a well-defined order. The detailed study of the folding dynamics of protein-like sequences designed as to exhibit different contact energy distributions, as well as different degrees of sequence optimization (i.e., participation of non-native interactions in the folding process), reveals significant differences in the corresponding locking scenarios—the collection of native contacts and their average locking times, which are largely ascribable to the dynamics of non-native contacts. Furthermore, strong evidence for a positive role played by non-native contacts at an early folding stage was also found. Interestingly, for topologically simple target structures, a positive interplay between native and non-native contacts is observed also toward the end of the folding process, suggesting that non-native contacts may indeed affect the overall folding process. For target models exhibiting clear two-state kinetics, the relation between the nucleation mechanism of folding and the locking scenario is investigated. Our results suggest that the stabilization of the folding transition state can be achieved through the establishment of a very small network of native contacts that are the first to lock during the folding process.
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Citations
Ubiquitin folds via a flip-twist-lock mechanism
TL;DR: The folding mechanism of a globular protein, ubiquitin, is reported from its chemically denatured state using all-atom molecular dynamics simulations and it is shown that ubiquitIn folds via an intermediate, and the presence of "biological water" is confirmed and explained.
De novo prediction of protein folding pathways and structure using the principle of sequential stabilization
TL;DR: A unified approach for predicting folding pathways and tertiary structure using only the primary sequence as input and can identify kinetically significant non-native interactions and intermediates, sometimes generated by only two mutations, while the evolution of contact matrices is often consistent with experiments.
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Effects of knot type in the folding of topologically complex lattice proteins.
TL;DR: The present study predicts that mutations that perturb the folding transition state may significantly enhance the kinetic stability of knotted proteins provided they involve residues located within the knotted core.
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