Protection of rhesus macaques against disease progression from pathogenic SHIV-89.6PD by vaccination with phage-displayed HIV-1 epitopes

Xueni Chen; Giuseppe Scala; Ileana Quinto; Weimin Liu; Tae Wook Chun; J. Shawn Justement; Oren J. Cohen; Tom C. Vancott; Marcin Iwanicki; Mark G. Lewis; Jack Greenhouse; Todd Barry; David Venzon; Anthony S. Fauci

doi:10.1038/nm1101-1225

Protection of rhesus macaques against disease progression from pathogenic SHIV-89.6PD by vaccination with phage-displayed HIV-1 epitopes

Xueni Chen, Giuseppe Scala, Ileana Quinto, Weimin Liu, Tae Wook Chun, J. Shawn Justement, Oren J. Cohen, Tom C. Vancott, Marcin Iwanicki, Mark G. Lewis, Jack Greenhouse, Todd Barry, David Venzon, Anthony S. Fauci

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

74 Scopus citations

Abstract

The antigenic polymorphism of HIV-1 is a major obstacle in developing an effective vaccine. Accordingly, we screened random peptide libraries (RPLs) displayed on phage with antibodies from HIV-infected individuals and identified an array of HIV-specific epitopes that behave as antigenic mimics of conformational epitopes of gp120 and gp41 proteins. We report that the selected epitopes are shared by a collection of HIV-1 isolates of clades A-F. The phage-borne epitopes are immunogenic in rhesus macaques, where they elicit envelope-specific antibody responses. Upon intravenous challenge with 60 MID₅₀ of pathogenic SHIV-89.6PD, all monkeys became infected; however, in contrast to the naive and mock-immunized monkeys, four of five mimotope-immunized monkeys experienced lower levels of peak viremia, followed by viral set points of undetectable or transient levels of viremia and a mild decline of CD4⁺ T cells, and were protected from progression to AIDS-like illness. These results provide a new approach to the design of broadly protective HIV-1 vaccines.

Original language	English
Pages (from-to)	1225-1231
Number of pages	7
Journal	Nature Medicine
Volume	7
Issue number	11
DOIs	https://doi.org/10.1038/nm1101-1225
State	Published - 2001

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Chen, X., Scala, G., Quinto, I., Liu, W., Chun, T. W., Shawn Justement, J., Cohen, O. J., Vancott, T. C., Iwanicki, M., Lewis, M. G., Greenhouse, J., Barry, T., Venzon, D., & Fauci, A. S. (2001). Protection of rhesus macaques against disease progression from pathogenic SHIV-89.6PD by vaccination with phage-displayed HIV-1 epitopes. Nature Medicine, 7(11), 1225-1231. https://doi.org/10.1038/nm1101-1225

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title = "Protection of rhesus macaques against disease progression from pathogenic SHIV-89.6PD by vaccination with phage-displayed HIV-1 epitopes",

abstract = "The antigenic polymorphism of HIV-1 is a major obstacle in developing an effective vaccine. Accordingly, we screened random peptide libraries (RPLs) displayed on phage with antibodies from HIV-infected individuals and identified an array of HIV-specific epitopes that behave as antigenic mimics of conformational epitopes of gp120 and gp41 proteins. We report that the selected epitopes are shared by a collection of HIV-1 isolates of clades A-F. The phage-borne epitopes are immunogenic in rhesus macaques, where they elicit envelope-specific antibody responses. Upon intravenous challenge with 60 MID50 of pathogenic SHIV-89.6PD, all monkeys became infected; however, in contrast to the naive and mock-immunized monkeys, four of five mimotope-immunized monkeys experienced lower levels of peak viremia, followed by viral set points of undetectable or transient levels of viremia and a mild decline of CD4+ T cells, and were protected from progression to AIDS-like illness. These results provide a new approach to the design of broadly protective HIV-1 vaccines.",

author = "Xueni Chen and Giuseppe Scala and Ileana Quinto and Weimin Liu and Chun, {Tae Wook} and {Shawn Justement}, J. and Cohen, {Oren J.} and Vancott, {Tom C.} and Marcin Iwanicki and Lewis, {Mark G.} and Jack Greenhouse and Todd Barry and David Venzon and Fauci, {Anthony S.}",

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Chen, X, Scala, G, Quinto, I, Liu, W, Chun, TW, Shawn Justement, J, Cohen, OJ, Vancott, TC, Iwanicki, M, Lewis, MG, Greenhouse, J, Barry, T, Venzon, D & Fauci, AS 2001, 'Protection of rhesus macaques against disease progression from pathogenic SHIV-89.6PD by vaccination with phage-displayed HIV-1 epitopes', Nature Medicine, vol. 7, no. 11, pp. 1225-1231. https://doi.org/10.1038/nm1101-1225

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AU - Chen, Xueni

AU - Scala, Giuseppe

AU - Quinto, Ileana

AU - Liu, Weimin

AU - Chun, Tae Wook

AU - Shawn Justement, J.

AU - Cohen, Oren J.

AU - Vancott, Tom C.

AU - Iwanicki, Marcin

AU - Lewis, Mark G.

AU - Greenhouse, Jack

AU - Barry, Todd

AU - Venzon, David

AU - Fauci, Anthony S.

PY - 2001

Y1 - 2001

N2 - The antigenic polymorphism of HIV-1 is a major obstacle in developing an effective vaccine. Accordingly, we screened random peptide libraries (RPLs) displayed on phage with antibodies from HIV-infected individuals and identified an array of HIV-specific epitopes that behave as antigenic mimics of conformational epitopes of gp120 and gp41 proteins. We report that the selected epitopes are shared by a collection of HIV-1 isolates of clades A-F. The phage-borne epitopes are immunogenic in rhesus macaques, where they elicit envelope-specific antibody responses. Upon intravenous challenge with 60 MID50 of pathogenic SHIV-89.6PD, all monkeys became infected; however, in contrast to the naive and mock-immunized monkeys, four of five mimotope-immunized monkeys experienced lower levels of peak viremia, followed by viral set points of undetectable or transient levels of viremia and a mild decline of CD4+ T cells, and were protected from progression to AIDS-like illness. These results provide a new approach to the design of broadly protective HIV-1 vaccines.

AB - The antigenic polymorphism of HIV-1 is a major obstacle in developing an effective vaccine. Accordingly, we screened random peptide libraries (RPLs) displayed on phage with antibodies from HIV-infected individuals and identified an array of HIV-specific epitopes that behave as antigenic mimics of conformational epitopes of gp120 and gp41 proteins. We report that the selected epitopes are shared by a collection of HIV-1 isolates of clades A-F. The phage-borne epitopes are immunogenic in rhesus macaques, where they elicit envelope-specific antibody responses. Upon intravenous challenge with 60 MID50 of pathogenic SHIV-89.6PD, all monkeys became infected; however, in contrast to the naive and mock-immunized monkeys, four of five mimotope-immunized monkeys experienced lower levels of peak viremia, followed by viral set points of undetectable or transient levels of viremia and a mild decline of CD4+ T cells, and were protected from progression to AIDS-like illness. These results provide a new approach to the design of broadly protective HIV-1 vaccines.

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Protection of rhesus macaques against disease progression from pathogenic SHIV-89.6PD by vaccination with phage-displayed HIV-1 epitopes

Abstract

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