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Integrated Prediction of Protein Struture at 1D, 2D and 3D Levels

$283,648R01FY2013GMNIH

University Of Missouri-Columbia, Columbia MO

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Abstract

DESCRIPTION (provided by applicant): Computational prediction of protein structure from the amino acid sequence is one of the most important and challenging problems in bioinformatics and computational biology. With the exponential growth of protein sequences without solved protein structures in the post-genomic era, accurate protein structure prediction methods and tools are in urgent need. Here, we propose to develop an integrated approach to advance protein structure prediction at the 1-dimensional (1D), 2-dimensional (2D) and 3-dimensional (3D) levels. At the 1D level, novel information such as domain evolution signals, alternative gene splicing sites, and 2D protein contact map will be used to predict protein domain boundaries from the sequences. At the 2D level, new methods such as residue contact propagation, machine learning boosting, linear programming, and Markov Chain Monte Carlo simulations will be used to advance residue-residue contact prediction for a domain, or a protein. At the 3D level, 2D contact prediction, fold recognition via machine learning, and multi-template combination will be used to enhance both template-based and ab initio structure prediction. Finally, knowledge-based statistical machine learning methods and model combination algorithms will be developed to reliably evaluate and refine the quality of predicted protein structural models. One of several innovative aspects of this approach is to integrate 1D, 2D, and 3D predictions in order to improve each other through protein structural unit - domains. The 1D, 2D, and 3D protein structure prediction methods will be implemented as user-friendly software packages and web services released to the scientific community. These tools and web services will be useful for protein structure prediction, structure determination, functional analysis, protein engineering, protein mutagenesis analysis, and protein design.

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