ASIA unversity:Item 310904400/101597
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    题名: Finding a Potential Dipeptidyl Peptidase-4 (DPP-4) Inhibitor for Type-2 Diabetes Treatment Based on Molecular Docking, Pharmacophore Generation, and Molecular Dynamics Simulation
    作者: Harika Meduru;王焰增;Wang, Yeng-Tseng;蔡進發;TSAI, JEFFREY J. P.;陳玉菁;CHEN, YU-CHING;*
    贡献者: 生物資訊與醫學工程學系
    日期: 2016-06
    上传时间: 2016-11-08 02:13:56 (UTC+0)
    摘要: Dipeptidyl peptidase-4 (DPP-4) is the vital enzyme that is responsible for inactivating intestinal peptides glucagon like peptide-1 (GLP-1) and Gastric inhibitory polypeptide (GIP), which stimulates a decline in blood glucose levels. The aim of this study was to explore the inhibition activity of small molecule inhibitors to DPP-4 following a computational strategy based on docking studies and molecular dynamics simulations. The thorough docking protocol we applied allowed us to derive good correlation parameters between the predicted binding affinities (pKi) of the DPP-4 inhibitors and the experimental activity values (pIC50). Based on molecular docking receptor-ligand interactions, pharmacophore generation was carried out in order to identify the binding modes of structurally diverse compounds in the receptor active site. Consideration of the permanence and flexibility of DPP-4 inhibitor complexes by means of molecular dynamics (MD) simulation specified that the inhibitors maintained the binding mode observed in the docking study. The present study helps generate new information for further structural optimization and can influence the development of new DPP-4 inhibitors discoveries in the treatment of type-2 diabetes.
    關聯: INTERNATIONAL JOURNAL OF MOLECULAR SCIENCES
    显示于类别:[生物資訊與醫學工程學系 ] 期刊論文

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