Alteration of V3 Loop Context Within the Envelope of Human Immunodeficiency Virus Type 1 Enhances Neutralization

Overview

Journal J Virol

Publisher American Society for Microbiology

Date 1994 Jun 1

PMID 7514675

Citations 3

Authors

M Robert-Guroff

A Louie

M Myagkikh

F Michaels

M P Kieny

M E White-Scharf

B Potts

D Grogg

M S Reitz Jr

Affiliations

Soon will be listed here.

Abstract

Neutralization of a chimeric human immunodeficiency virus (HIV) type 1, containing the V3 loop of the MN isolate substituted within the HXB2 envelope, was enhanced up to 20-fold compared with the HXB2 or MN parental isolates by human HIV-positive sera. MN V3 loop-specific monoclonal antibodies were better able to recognize the chimeric virus compared with MN, staining a greater percentage of infected cells and exhibiting slight increases in relative affinity with a concomitant increase in neutralization titer. Competition analysis revealed that enhanced neutralization by human HIV-positive sera of the chimera was attributable in some cases to better reactivity with the linear V3 loop epitope but in others to conformational loop epitopes or previously cryptic or poorly recognized epitopes outside the loop region. Mice primed with a vaccinia virus-chimeric envelope recombinant and boosted with gp160 developed a spectrum of antibodies different from that of mice similarly immunized with HXB2 or MN recombinants or that of naturally infected humans. The chimeric envelope elicited antibodies with enhanced binding to the native MN V3 loop; however, the sites seen by the BALB/c mice were not neutralizing epitopes. Nevertheless, similar to the observations made with use of human sera, the chimeric virus was more readily neutralized by all of the immune mouse sera, an effect apparently mediated by non-V3 loop epitopes. These studies illustrate that not only the V3 loop sequence and conformation but also its context within the viral envelope influence neutralization.

Citing Articles

Spontaneous reversion of human immunodeficiency virus type 1 neutralization-resistant variant HXB2thr582: in vitro selection against cytopathicity highlights gp120-gp41 interactive regions.

Stern T, Reitz Jr M, Robert-Guroff M J Virol. 1995; 69(3):1860-7.

PMID: 7853527 PMC: 188797. DOI: 10.1128/JVI.69.3.1860-1867.1995.

An infectious chimeric human immunodeficiency virus type 2 (HIV-2) expressing the HIV-1 principal neutralizing determinant.

Mamounas M, Looney D, Talbott R, Wong-Staal F J Virol. 1995; 69(10):6424-9.

PMID: 7666543 PMC: 189542. DOI: 10.1128/JVI.69.10.6424-6429.1995.

Insertion of primary syncytium-inducing (SI) and non-SI envelope V3 loops in human immunodeficiency virus type 1 (HIV-1) LAI reduces neutralization sensitivity to autologous, but not heterologous, HIV-1 antibodies.

Hogervorst E, de Jong J, van Wijk A, Bakker M, Valk M, Nara P J Virol. 1995; 69(10):6342-51.

PMID: 7666535 PMC: 189533. DOI: 10.1128/JVI.69.10.6342-6351.1995.

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