Broadly cross-reactive HIV neutralizing human monoclonal antibody Fab selected by sequential antigen panning of a phage display library

Mei Yun Zhang; Yuuei Shu; Sanjay Phogat; Xiaodong Xiao; Fatim Cham; Peter Bouma; Anil Choudhary; Yan Ru Feng; Inaki Sanz; Susanna Rybak; Christopher C. Broder; Gerald V. Quinnan; Thomas Evans; Dimiter S. Dimitrov

doi:10.1016/j.jim.2003.07.003

Broadly cross-reactive HIV neutralizing human monoclonal antibody Fab selected by sequential antigen panning of a phage display library

Mei Yun Zhang, Yuuei Shu, Sanjay Phogat, Xiaodong Xiao, Fatim Cham, Peter Bouma, Anil Choudhary, Yan Ru Feng, Inaki Sanz, Susanna Rybak, Christopher C. Broder, Gerald V. Quinnan, Thomas Evans, Dimiter S. Dimitrov^*

^*Corresponding author for this work

Microbiology and Immunology

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

66 Scopus citations

Abstract

Identification of broadly cross-reactive human monoclonal antibodies (mAbs) has major implications for development of vaccines, inhibitors and research tools. Here we describe a sequential antigen panning (SAP) methodology that may facilitate the selection of such antibodies. An HIV-specific antibody Fab (m18) was selected from a human Fab phage-display library by SAP against several recombinant soluble HIV envelope glycoproteins (Envs) and Env-sCD4 complexes. This Fab bound to a variety of recombinant soluble Envs (gp140s) from primary HIV isolates representing different clades, and inhibited cell fusion and virus entry mediated by Envs of primary HIV isolates. The methodology and the results may have implications for development of HIV vaccines and inhibitors, as well as for identification of antibodies to conserved epitopes on rapidly mutating viruses and cells.

Original language	English
Pages (from-to)	17-25
Number of pages	9
Journal	Journal of Immunological Methods
Volume	283
Issue number	1-2
DOIs	https://doi.org/10.1016/j.jim.2003.07.003
State	Published - Dec 2003

Keywords

Antibody
gp120
HIV
Inhibitors
Phage display
Vaccines

Access to Document

10.1016/j.jim.2003.07.003

Cite this

Zhang, M. Y., Shu, Y., Phogat, S., Xiao, X., Cham, F., Bouma, P., Choudhary, A., Feng, Y. R., Sanz, I., Rybak, S., Broder, C. C., Quinnan, G. V., Evans, T., & Dimitrov, D. S. (2003). Broadly cross-reactive HIV neutralizing human monoclonal antibody Fab selected by sequential antigen panning of a phage display library. Journal of Immunological Methods, 283(1-2), 17-25. https://doi.org/10.1016/j.jim.2003.07.003

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abstract = "Identification of broadly cross-reactive human monoclonal antibodies (mAbs) has major implications for development of vaccines, inhibitors and research tools. Here we describe a sequential antigen panning (SAP) methodology that may facilitate the selection of such antibodies. An HIV-specific antibody Fab (m18) was selected from a human Fab phage-display library by SAP against several recombinant soluble HIV envelope glycoproteins (Envs) and Env-sCD4 complexes. This Fab bound to a variety of recombinant soluble Envs (gp140s) from primary HIV isolates representing different clades, and inhibited cell fusion and virus entry mediated by Envs of primary HIV isolates. The methodology and the results may have implications for development of HIV vaccines and inhibitors, as well as for identification of antibodies to conserved epitopes on rapidly mutating viruses and cells.",

keywords = "Antibody, gp120, HIV, Inhibitors, Phage display, Vaccines",

author = "Zhang, {Mei Yun} and Yuuei Shu and Sanjay Phogat and Xiaodong Xiao and Fatim Cham and Peter Bouma and Anil Choudhary and Feng, {Yan Ru} and Inaki Sanz and Susanna Rybak and Broder, {Christopher C.} and Quinnan, {Gerald V.} and Thomas Evans and Dimitrov, {Dimiter S.}",

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Zhang, MY, Shu, Y, Phogat, S, Xiao, X, Cham, F, Bouma, P, Choudhary, A, Feng, YR, Sanz, I, Rybak, S, Broder, CC, Quinnan, GV, Evans, T & Dimitrov, DS 2003, 'Broadly cross-reactive HIV neutralizing human monoclonal antibody Fab selected by sequential antigen panning of a phage display library', Journal of Immunological Methods, vol. 283, no. 1-2, pp. 17-25. https://doi.org/10.1016/j.jim.2003.07.003

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AU - Zhang, Mei Yun

AU - Shu, Yuuei

AU - Phogat, Sanjay

AU - Xiao, Xiaodong

AU - Cham, Fatim

AU - Bouma, Peter

AU - Choudhary, Anil

AU - Feng, Yan Ru

AU - Sanz, Inaki

AU - Rybak, Susanna

AU - Broder, Christopher C.

AU - Quinnan, Gerald V.

AU - Evans, Thomas

AU - Dimitrov, Dimiter S.

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AB - Identification of broadly cross-reactive human monoclonal antibodies (mAbs) has major implications for development of vaccines, inhibitors and research tools. Here we describe a sequential antigen panning (SAP) methodology that may facilitate the selection of such antibodies. An HIV-specific antibody Fab (m18) was selected from a human Fab phage-display library by SAP against several recombinant soluble HIV envelope glycoproteins (Envs) and Env-sCD4 complexes. This Fab bound to a variety of recombinant soluble Envs (gp140s) from primary HIV isolates representing different clades, and inhibited cell fusion and virus entry mediated by Envs of primary HIV isolates. The methodology and the results may have implications for development of HIV vaccines and inhibitors, as well as for identification of antibodies to conserved epitopes on rapidly mutating viruses and cells.

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