NDLI: Molecular dynamics simulation and free energy calculation studies of kinase inhibitors binding to active and inactive conformations of VEGFR-2.

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Molecular dynamics simulation and free energy calculation studies of kinase inhibitors binding to active and inactive conformations of VEGFR-2.

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Molecular dynamics simulation and free energy calculation studies of kinase inhibitors binding to active and inactive conformations of VEGFR-2.

Content Provider	World Health Organization (WHO)-Global Index Medicus
Author	Wu, XiaoYun Wan, ShanHe Wang, GuangFa Jin, Hong Li, ZhongHuang Tian, YuanXin Zhu, ZhengGuang Zhang, JiaJie
Description	Author Affiliation: Wu X ( School of Pharmaceutical Sciences, Southern Medical University, Guangzhou 510515, PR China. Electronic address: xywugz@163.com.); Wan S ( School of Pharmaceutical Sciences, Southern Medical University, Guangzhou 510515, PR China.); Wang G ( School of Pharmaceutical Sciences, Southern Medical University, Guangzhou 510515, PR China.); Jin H ( School of Pharmaceutical Sciences, Southern Medical University, Guangzhou 510515, PR China.); Li Z ( School of Pharmaceutical Sciences, Southern Medical University, Guangzhou 510515, PR China.); Tian Y ( School of Pharmaceutical Sciences, Southern Medical University, Guangzhou 510515, PR China.); Zhu Z ( School of Pharmaceutical Sciences, Southern Medical University, Guangzhou 510515, PR China.); Zhang J ( School of Pharmaceutical Sciences, Southern Medical University, Guangzhou 510515, PR China. Electronic address: zhangjj@smu.edu.cn.)
Abstract	Vascular endothelial growth factors receptor-2 (VEGFR-2) inhibitors have been proved as very effective anticancer agents. Structurally similar ligands 1 and 2 show almost the same inhibitory activities against VEGFR-2, but they bind to the enzyme in distinct binding mode. Ligand 1 targets DFG-in active conformation of VEGFR-2, known as Type I inhibitor. On the other hand, ligand 2 targets DFG-out inactive conformation of VEGFR-2, known as Type II inhibitor or allosteric kinase inhibitor. Ligand 2 shows high inhibitory activity, while the compound 3, a close analog of 2 with the cyclopropylamide replaced by tert-butylamide, exhibits drastically diminished potency. In this work, molecular dynamics simulations and free energy calculations were performed on inhibitors 1-3 binding to active and inactive conformation of VEGFR-2. Molecular dynamics simulations find that the active conformation binding to Type I inhibitor 1 appears more flexible when compared to the unbound form. In contrast, binding of Type II inhibitor 2 to the inactive conformation helps to stabilize the inactive conformation of the protein. Binding free energy calculations verify that inhibitors 1 and 2 have almost the same activities against VEGFR-2, and that ligand 1 binds to and stabilizes the DFG-in conformation of VEGFR-2, which is in agree with the experimental observation. Molecular dynamics simulations and binding free energy calculations of 3 binding to VEGFR-2 can give a good explanation of the drastically diminished potency. Free energy analysis revealed that van der Waals interactions provided the substantial driving force for the binding process. The important hydrophobic property of the terminal 4-Cl phenyl was required to be Type II inhibitors. Furthermore, per-residue free energy decomposition analysis revealed that the most favorable contribution came from Leu840, Val848, Ala866, Lys868, Leu889, Val899, Thr916, Phe918, Cys919, Leu1035, Cys1045, Asp1046, and Phe1047. These results are expected to be useful for future rational design of novel potent VEGFR-2 inhibitors.
File Format	HTM / HTML
ISSN	10933263
Volume Number	56
e-ISSN	18734243
Journal	Journal of Molecular Graphics and Modelling
Language	English
Publisher	Elsevier
Publisher Date	2015-03-01
Publisher Place	United States
Access Restriction	One Nation One Subscription (ONOS)
Subject Keyword	Discipline Molecular Biology Molecular Docking Simulation Protein Kinase Inhibitors Chemistry Vascular Endothelial Growth Factor Receptor-2 Allosteric Regulation Amino Acid Motifs Binding Sites Humans Hydrophobic And Hydrophilic Interactions Kinetics Ligands Molecular Sequence Data Protein Binding Protein Conformation Structure-activity Relationship Thermodynamics Antagonists & Inhibitors Journal Article Research Support, Non-u.s. Gov't
Content Type	Text
Resource Type	Article
Subject	Computer Graphics and Computer-Aided Design Spectroscopy Materials Chemistry Physical and Theoretical Chemistry

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