標題: GEMDOCK: A generic evolutionary method for molecular docking
作者: Yang, JM
Chen, CC
生物科技學系
Department of Biological Science and Technology
關鍵字: cross-docking;evolutionary algorithm;molecular recognition;protein-ligand docking;hybrid docking;structure-based drug design
公開日期: 1-五月-2004
摘要: We have developed an evolutionary approach for flexible ligand docking. This approval, GEMDOCK, uses a Generic Evolutionary Method for molecular DOCKing and an empirical scoring function. The former combines both discrete and continuous global search strategies with local search strategies to speed up convergence, whereas the latter results in rapid recognition of potential ligands. GEMDOCK was tested on a diverse data set of 100 protein-ligand complexes from the Protein Data Bank. In 79% of these complexes, the docked lowest energy ligand structures had root-mean-square derivations (RMSDs) below 2.0 Angstrom with respect to the corresponding crystal structures. The success rate increased to 85% if the structure water molecules were retained. We evaluated GEMDOCK on two cross-docking experiments in which each ligand of a protein ensemble was docked into each protein of the ensemble. Seventy-six percent of the docked structures had RMSDs below 2.0 Angstrom when the ligands were docked into foreign structures. We analyzed and validated GEMDOCK with respect to various search spaces and scoring functions, and found that if the scoring function was perfect, then the predicted accuracy was also essentially perfect. This study suggests that GEMDOCK is a useful tool for molecular recognition and may be used to systematically evaluate and thus improve scoring functions. (C) 2004 Wiley-Liss, Inc.
URI: http://dx.doi.org/10.1002/prot.20035
http://hdl.handle.net/11536/26795
ISSN: 0887-3585
DOI: 10.1002/prot.20035
期刊: PROTEINS-STRUCTURE FUNCTION AND BIOINFORMATICS
Volume: 55
Issue: 2
起始頁: 288
結束頁: 304
顯示於類別:期刊論文


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