RIGID-BODY DOCKING WITH MUTANT CONSTRAINTS OF INFLUENZA HEMAGGLUTININ WITH ANTIBODY HC19
被引:28
作者:
CHERFILS, J
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UNIV PARIS SUD,BIOL STRUCT LAB,CNRS,UMR 9920,F-91198 GIF SUR YVETTE,FRANCEUNIV PARIS SUD,BIOL STRUCT LAB,CNRS,UMR 9920,F-91198 GIF SUR YVETTE,FRANCE
CHERFILS, J
[1
]
BIZEBARD, T
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UNIV PARIS SUD,BIOL STRUCT LAB,CNRS,UMR 9920,F-91198 GIF SUR YVETTE,FRANCEUNIV PARIS SUD,BIOL STRUCT LAB,CNRS,UMR 9920,F-91198 GIF SUR YVETTE,FRANCE
BIZEBARD, T
[1
]
KNOSSOW, M
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UNIV PARIS SUD,BIOL STRUCT LAB,CNRS,UMR 9920,F-91198 GIF SUR YVETTE,FRANCEUNIV PARIS SUD,BIOL STRUCT LAB,CNRS,UMR 9920,F-91198 GIF SUR YVETTE,FRANCE
KNOSSOW, M
[1
]
JANIN, J
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UNIV PARIS SUD,BIOL STRUCT LAB,CNRS,UMR 9920,F-91198 GIF SUR YVETTE,FRANCEUNIV PARIS SUD,BIOL STRUCT LAB,CNRS,UMR 9920,F-91198 GIF SUR YVETTE,FRANCE
JANIN, J
[1
]
机构:
[1] UNIV PARIS SUD,BIOL STRUCT LAB,CNRS,UMR 9920,F-91198 GIF SUR YVETTE,FRANCE
来源:
PROTEINS-STRUCTURE FUNCTION AND GENETICS
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1994年
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18卷
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01期
An automatic docking algorithm has been applied to the modeling of the complex between hemagglutinin from influenza virus and the Fab fragment of a monoclonal antibody raised against this antigen. We have introduced here the use of biochemical information provided by mutants of hemagglutinin. The docking procedure finds a small number of candidate solutions where three sites of escape mutations are buried and form hydrogen bonds in the interface. The localization of the epitope is improved by additional biochemical data about mutants that do not affect antibody binding. Five candidate solutions with low energy, reasonably well-packed interfaces, and six to ten hydrogen bonds are compatible with mutant information. One of the five stands out as generally better than the others from these points of views. (C) 1994 Wiley-Liss, Inc.