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The use of soluble protein structures in modeling helical proteins in a layered membrane
Authors:Hong Wing Lee  Hong Ching Lee  Lawrence K Lee  Erdahl T Teber
Institution:1. Faculty of Pharmacy, Group in Biomolecular Structure and Informatics, University of Sydney, Sydney, NSW, 2006, Australia.;2. Computational and Structural Biology Division, Victor Chang Cardiac Research Institute, Sydney, NSW, 2010, Australia.;3. Children’s Medical Research Institute, 214 Hawkesbury Road, Westmead, NSW, 2145, Australia.
Abstract:Major advances have been made in the prediction of soluble protein structures, led by the knowledge-based modeling methods that extract useful structural trends from known protein structures and incorporate them into scoring functions. The same cannot be reported for the class of transmembrane proteins, primarily due to the lack of high-resolution structural data for transmembrane proteins, which render many of the knowledge-based method unreliable or invalid. We have developed a method that harnesses the vast structural knowledge available in soluble protein data for use in the modeling of transmembrane proteins. At the core of the method, a set of transmembrane protein decoy sets that allow us to filter and train features recognized from soluble proteins for transmembrane protein modeling into a set of scoring functions. We have demonstrated that structures of soluble proteins can provide significant insight into transmembrane protein structures. A complementary novel two-stage modeling/selection process that mimics the two-stage helical membrane protein folding was developed. Combined with the scoring function, the method was successfully applied to model 5 transmembrane proteins. The root mean square deviations of the predicted models ranged from 5.0 to 8.8?Å to the native structures.
Keywords:protein structure  polytopic membrane proteins  knowledge-based modeling  structural bioinformatics
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