Probing the HIV gp120 envelope glycoprotein conformation by NMR

Jessica Celigoy; Benjamin Ramirez; Lin Tao; Lijun Rong; Lianying Yan; Yan Ru Feng; Gerald V. Quinnan; Christopher C. Broder; Michael Caffrey

doi:10.1074/jbc.M111.251025

Probing the HIV gp120 envelope glycoprotein conformation by NMR

Jessica Celigoy, Benjamin Ramirez, Lin Tao, Lijun Rong, Lianying Yan, Yan Ru Feng, Gerald V. Quinnan, Christopher C. Broder, Michael Caffrey^*

^*Corresponding author for this work

Microbiology and Immunology

Research output: Contribution to journal › Article › peer-review

14 Scopus citations

Abstract

The HIV envelope glycoprotein gp120 plays a critical role in virus entry, and thus, its structure is of extreme interest for the development of novel therapeutics and vaccines. To date, high resolution structural information about gp120 in complex with gp41 has proven intractable. In this study, we characterize the structural properties of gp120 in the presence and absence of gp41 domains by NMR. Using the peptide probe 12p1 (sequence, RINNIPWSEAMM), which was identified previously as an entry inhibitor that binds to gp120, we identify atoms of 12p1 in close contact with gp120 in the monomeric and trimeric states. Interestingly, the binding mode of 12p1 with gp120 is similar for clades B and C. In addition, we show a subtle difference in the binding mode of 12p1 in the presence of gp41 domains, i.e. the trimeric state, which we interpret as small differences in the gp120 structure in the presence of gp41.

Original language	English
Pages (from-to)	23975-23981
Number of pages	7
Journal	Journal of Biological Chemistry
Volume	286
Issue number	27
DOIs	https://doi.org/10.1074/jbc.M111.251025
State	Published - 8 Jul 2011

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10.1074/jbc.M111.251025

Cite this

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title = "Probing the HIV gp120 envelope glycoprotein conformation by NMR",

abstract = "The HIV envelope glycoprotein gp120 plays a critical role in virus entry, and thus, its structure is of extreme interest for the development of novel therapeutics and vaccines. To date, high resolution structural information about gp120 in complex with gp41 has proven intractable. In this study, we characterize the structural properties of gp120 in the presence and absence of gp41 domains by NMR. Using the peptide probe 12p1 (sequence, RINNIPWSEAMM), which was identified previously as an entry inhibitor that binds to gp120, we identify atoms of 12p1 in close contact with gp120 in the monomeric and trimeric states. Interestingly, the binding mode of 12p1 with gp120 is similar for clades B and C. In addition, we show a subtle difference in the binding mode of 12p1 in the presence of gp41 domains, i.e. the trimeric state, which we interpret as small differences in the gp120 structure in the presence of gp41.",

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AU - Celigoy, Jessica

AU - Ramirez, Benjamin

AU - Tao, Lin

AU - Rong, Lijun

AU - Yan, Lianying

AU - Feng, Yan Ru

AU - Quinnan, Gerald V.

AU - Broder, Christopher C.

AU - Caffrey, Michael

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AB - The HIV envelope glycoprotein gp120 plays a critical role in virus entry, and thus, its structure is of extreme interest for the development of novel therapeutics and vaccines. To date, high resolution structural information about gp120 in complex with gp41 has proven intractable. In this study, we characterize the structural properties of gp120 in the presence and absence of gp41 domains by NMR. Using the peptide probe 12p1 (sequence, RINNIPWSEAMM), which was identified previously as an entry inhibitor that binds to gp120, we identify atoms of 12p1 in close contact with gp120 in the monomeric and trimeric states. Interestingly, the binding mode of 12p1 with gp120 is similar for clades B and C. In addition, we show a subtle difference in the binding mode of 12p1 in the presence of gp41 domains, i.e. the trimeric state, which we interpret as small differences in the gp120 structure in the presence of gp41.

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