Factors Determining the Breadth and Potency of Neutralization by V3-Specific Human Monoclonal Antibodies Derived from Subjects Infected with Clade A or Clade B Strains of Human Immunodeficiency Virus Type 1

Author:

Krachmarov C. P.1,Honnen W. J.1,Kayman S. C.1,Gorny M. K.2,Zolla-Pazner S.23,Pinter Abraham14

Affiliation:

1. Public Health Research Institute, Newark, New Jersey

2. NYU School of Medicine, New York, New York

3. New York Veterans Affairs Medical Center, New York, New York

4. Department of Medicine, New Jersey Medical School, UMDNJ, Newark, New Jersey

Abstract

ABSTRACT The neutralizing activities of anti-V3 antibodies for HIV-1 isolates is affected both by sequence variation within V3 and by epitope masking by the V1/V2 domain. To analyze the relative contribution of V3 sequence variation, chimeric Env genes that contained consensus V3 sequences from seven HIV-1 subtypes in the neutralization-sensitive SF162 Env backbone were constructed. Resulting viral pseudotypes were tested for neutralization by 15 anti-V3 MAbs isolated from humans infected with viruses of either subtype B (anti-V3 B MAbs) or subtype A (anti-V3 A MAbs). Pseudovirions with the subtype B consensus V3 sequence were potently neutralized (IC 50 < 0.006 μg/ml) by all but one of these MAbs, while pseudovirions with V3 subtypes A, C, F, H, AG, and AE were generally neutralized more effectively by anti-V3 A MAbs than by anti-V3 B MAbs. A V1/V2-masked Env version of SF162 Env with the consensus B V3 sequence was also neutralized by these MAbs, although with considerably lower potency, while similarly masked chimeras with V3 sequences of subtype A, C, or AG were weakly neutralized by anti-V3 A MAbs but not by anti-V3 B MAbs. Mutations in the V1/V2 domain of YU-2 Env increased the sensitivity of this highly resistant Env to a pool of anti-V3 B MAbs several thousand-fold. These results demonstrated (i) the exceptional sensitivity of representative V3 domains of multiple subtypes to neutralization in the absence of epitope masking, (ii) the broader neutralizing activity of anti-V3 A MAbs for viruses containing diverse V3 sequences, and (iii) the generality and dominant effect of V1/V2 masking on restriction of V3-mediated neutralization.

Publisher

American Society for Microbiology

Subject

Virology,Insect Science,Immunology,Microbiology

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