Title of article
Determination of the Transition State Ensemble for the Folding of Ubiquitin from a Combination of Φ and Ψ Analyses
Author/Authors
Péter V?rnai، نويسنده , , Christopher M. Dobson، نويسنده , , Michele Vendruscolo، نويسنده ,
Issue Information
روزنامه با شماره پیاپی سال 2008
Pages
14
From page
575
To page
588
Abstract
Protein engineering techniques have emerged as powerful tools for characterizing transition states (TSs) for protein folding. Recently, the Ψ analysis, in which double-histidine mutations create the possibility of reversible crosslinking in the native state, has been proposed as an additional approach to the well-established Φ analysis. We present here a combination of these two procedures for defining the structure of the TS of ubiquitin, a small α/β protein that has been used extensively as a model system for both experimental and computational studies of the protein-folding process. We performed a series of molecular dynamics simulations in which Φ and Ψ values were used as ensemble-averaged structural restraints to determine an ensemble of structures representing the TS of ubiquitin. Although the available Ψ values for ubiquitin did not, by themselves, generate well-defined TS ensembles, the inclusion of the restricted set of zero or unity values, but not fractional ones, provided useful complementary information to the Φ analysis. Our results show that the TS of ubiquitin is formed by a relatively narrow ensemble of structures exhibiting an overall native-like topology in which the N-terminal and C-terminal regions are in close proximity.
Keywords
psi values , transition state , Molecular dynamics , Protein folding , phi values
Journal title
Journal of Molecular Biology
Serial Year
2008
Journal title
Journal of Molecular Biology
Record number
1256407
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