Computational study of bindings of HK20 Fab and D5 Fab to HIV-1 gp41

Computational study of bindings of HK20 Fab and D5 Fab to HIV-1 gp41

Antibodies HK20 and D5 have been shown to target HIV-1 gp41, thereby inhibiting membrane fusion that facilitates viral entry. The binding picture is static, based on the X-ray crystal structures of the Fab regions and gp41 mimetic five-helix bundle. In this study, we carried out molecular dynamics s...

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Main Authors: Hartono, Yossa Dwi, Lazim, Raudah, Yip, Yew Mun, Zhang, Dawei
Other Authors: School of Physical and Mathematical Sciences
Format: Article
Language:English
Published: 2013
Online Access:https://hdl.handle.net/10356/99036
http://hdl.handle.net/10220/12790
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Institution: Nanyang Technological University
Language: English
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spelling sg-ntu-dr.10356-990362020-03-07T12:34:45Z Computational study of bindings of HK20 Fab and D5 Fab to HIV-1 gp41 Hartono, Yossa Dwi Lazim, Raudah Yip, Yew Mun Zhang, Dawei School of Physical and Mathematical Sciences Antibodies HK20 and D5 have been shown to target HIV-1 gp41, thereby inhibiting membrane fusion that facilitates viral entry. The binding picture is static, based on the X-ray crystal structures of the Fab regions and gp41 mimetic five-helix bundle. In this study, we carried out molecular dynamics simulation to provide the dynamic binding picture. Calculated binding free energies are within reasonable range of and follow the trend of the experimental values: −15.28 kcal/mol for HK20 Fab (expt. −11.60 kcal/mol) and −17.90 kcal/mol for D5 Fab (expt. −11.70 kcal/mol). Alanine scanning at protein–protein interface reveals that the highest contributors to binding for HK20 Fab are F54 and I56, both of VH region, as well as R30′ of VL region; whereas for D5 Fab, F54 of VH region, as well as W32′ and Y94′ of VL region. HK20 F54 and I56, as well as D5 I52, F54, and T56, bind to the gp41 hydrophobic binding pocket, an important region targeted by many other fusion inhibitors. Hydrogen bonding analysis also identifies high-occupancy hydrogen bonds at the periphery of gp41 hydrophobic pocket. Considering that almost all interface residues are turn residues, further work may be directed to turn mimics. Pre-orientation by the hydrogen bonds to poise this particular turn towards the binding pocket may also be a point worth pursuing. 2013-08-01T04:33:40Z 2019-12-06T20:02:33Z 2013-08-01T04:33:40Z 2019-12-06T20:02:33Z 2012 2012 Journal Article Hartono, Y. D., Lazim, R., Yip, Y. M.,& Zhang, D. (2012). Computational study of bindings of HK20 Fab and D5 Fab to HIV-1 gp41. Bioorganic & Medicinal Chemistry Letters, 22(4), 1695-1700. 0960-894X https://hdl.handle.net/10356/99036 http://hdl.handle.net/10220/12790 10.1016/j.bmcl.2011.12.105 en Bioorganic & medicinal chemistry letters
institution Nanyang Technological University
building NTU Library
country Singapore
collection DR-NTU
language English
description Antibodies HK20 and D5 have been shown to target HIV-1 gp41, thereby inhibiting membrane fusion that facilitates viral entry. The binding picture is static, based on the X-ray crystal structures of the Fab regions and gp41 mimetic five-helix bundle. In this study, we carried out molecular dynamics simulation to provide the dynamic binding picture. Calculated binding free energies are within reasonable range of and follow the trend of the experimental values: −15.28 kcal/mol for HK20 Fab (expt. −11.60 kcal/mol) and −17.90 kcal/mol for D5 Fab (expt. −11.70 kcal/mol). Alanine scanning at protein–protein interface reveals that the highest contributors to binding for HK20 Fab are F54 and I56, both of VH region, as well as R30′ of VL region; whereas for D5 Fab, F54 of VH region, as well as W32′ and Y94′ of VL region. HK20 F54 and I56, as well as D5 I52, F54, and T56, bind to the gp41 hydrophobic binding pocket, an important region targeted by many other fusion inhibitors. Hydrogen bonding analysis also identifies high-occupancy hydrogen bonds at the periphery of gp41 hydrophobic pocket. Considering that almost all interface residues are turn residues, further work may be directed to turn mimics. Pre-orientation by the hydrogen bonds to poise this particular turn towards the binding pocket may also be a point worth pursuing.
author2 School of Physical and Mathematical Sciences
author_facet School of Physical and Mathematical Sciences
Hartono, Yossa Dwi
Lazim, Raudah
Yip, Yew Mun
Zhang, Dawei
format Article
author Hartono, Yossa Dwi
Lazim, Raudah
Yip, Yew Mun
Zhang, Dawei
spellingShingle Hartono, Yossa Dwi
Lazim, Raudah
Yip, Yew Mun
Zhang, Dawei
Computational study of bindings of HK20 Fab and D5 Fab to HIV-1 gp41
author_sort Hartono, Yossa Dwi
title Computational study of bindings of HK20 Fab and D5 Fab to HIV-1 gp41
title_short Computational study of bindings of HK20 Fab and D5 Fab to HIV-1 gp41
title_full Computational study of bindings of HK20 Fab and D5 Fab to HIV-1 gp41
title_fullStr Computational study of bindings of HK20 Fab and D5 Fab to HIV-1 gp41
title_full_unstemmed Computational study of bindings of HK20 Fab and D5 Fab to HIV-1 gp41
title_sort computational study of bindings of hk20 fab and d5 fab to hiv-1 gp41
publishDate 2013
url https://hdl.handle.net/10356/99036
http://hdl.handle.net/10220/12790
_version_ 1681039251331874816

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