Ligand-protein docking studies of potential HIV-1 drug compounds using the algorithm FlexX

Patargias G.; Ewart G.; Luscombe C.Fischer W.B.

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Ligand-protein docking studies of potential HIV-1 drug compounds using the algorithm FlexX

机译：Ligand-protein docking studies of potential HIV-1 drug compounds using the algorithm FlexX

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摘要

Four compounds are docked to a pentameric bundle representing the transmembrane part of the Vpu protein from HIV-1. Employing the docking algorithm FlexX, their free energy of binding is estimated leading to the conclusion that potential drug candidates need to form H-bonds either with neighbouring or with n + 2 helices at the site of the serines within the bundle.

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来源
《Analytical and bioanalytical chemistry》 |2010年第7期|2559-2563|共5页
作者
Patargias G.; Ewart G.; Luscombe C.Fischer W.B.;
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作者单位

Biomembrane Structure Unit, Department of Biochemistry, Oxford University, South Parks Road, Oxford OX1 3QU, United Kingdom;

Biotron Limited, Suite 1.9, 56 Delhi Rd, North Ryde, NSW 2113, Australia;

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原文格式 PDF
正文语种英语
中图分类分析化学;
关键词
Docking approach; HIV-1; Ligand binding; Viral membrane proteins; Vpu;

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Ligand-protein docking studies of potential HIV-1 drug compounds using the algorithm FlexX

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