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    Please use this identifier to cite or link to this item: http://asiair.asia.edu.tw/ir/handle/310904400/16604

    Title: Computational analysis of de novo evolution of hepatitis C virus NS5B polymerase inhibitors
    Authors: 鍾景光;Chung, Jing-Gung
    Contributors: 生物科技學系
    Date: 2011-04
    Issue Date: 2012-11-23 17:15:00 (UTC+8)
    Abstract: HCV (Hepatitis C virus) that causes chronic liver disease. HCV NS5B RNA-dependent RNA polymerase (RbRp) and NS3 protease are able to affect virtual replication of genes. Computer-aided drug design (CADD) aims at designing new molecules with pharmacological activity. In this study, we used the Discovery Studio 2.0 program and the scoring function to estimate the Dock Score, piecewise linear potential 1 (PLP1), piecewise linear potential 2 (PLP2), and potential of mean force (PMF) score of novel compounds. In this way, novel compounds with "de novo evolution" can be found. Using the the pharmacophore features that are near the receptor pocket and the score functions to calculate scores for the ligand-receptor interaction, the new ligands were selected, developed and virtually placed in the binding site of the receptor. A new compound, EVO12, gave the best score, indicating that it may be an efficient polymerase inhibitor of HCV NS5B.
    Relation: IN VIVO, 25(2):219-228.
    Appears in Collections:[生物科技學系] 期刊論文

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