Initial antibodies binding to HIV-1 gp41 in acutely infected subjects are polyreactive and highly mutated

Author:

Liao Hua-Xin11,Chen Xi1,Munshaw Supriya1,Zhang Ruijun1,Marshall Dawn J.1,Vandergrift Nathan11,Whitesides John F.11,Lu Xiaozhi1,Yu Jae-Sung11,Hwang Kwan-Ki1,Gao Feng11,Markowitz Martin2,Heath Sonya L.3,Bar Katharine J.3,Goepfert Paul A.3,Montefiori David C.1,Shaw George C.3,Alam S. Munir11,Margolis David M.4,Denny Thomas N.11,Boyd Scott D.5,Marshal Eleanor5,Egholm Michael6,Simen Birgitte B.6,Hanczaruk Bozena6,Fire Andrew Z.5,Voss Gerald7,Kelsoe Garnett1,Tomaras Georgia D.111,Moody M. Anthony11,Kepler Thomas B.11,Haynes Barton F.111

Affiliation:

1. Duke Human Vaccine Institute, Department of Medicine, Department of Pediatrics, Department of Surgery, Department of Immunology, and Center for Computational Immunology, Duke University School of Medicine, Durham, NC 27710

2. The Aaron Diamond AIDS Research Center, New York, NY 10016

3. University of Alabama-Birmingham, Birmingham, AL 35294

4. University of North Carolina at Chapel Hill, Chapel Hill, NC 27599

5. Department of Pathology, Stanford School of Medicine, Stanford, CA 94305

6. 454 Life Sciences, Branford, CT 06405

7. GlaxoSmithKline Biologicals, 1330 Rixensart, Belgium

Abstract

The initial antibody response to HIV-1 is targeted to envelope (Env) gp41, and is nonneutralizing and ineffective in controlling viremia. To understand the origins and characteristics of gp41-binding antibodies produced shortly after HIV-1 transmission, we isolated and studied gp41-reactive plasma cells from subjects acutely infected with HIV-1. The frequencies of somatic mutations were relatively high in these gp41-reactive antibodies. Reverted unmutated ancestors of gp41-reactive antibodies derived from subjects acutely infected with HIV-1 frequently did not react with autologous HIV-1 Env; however, these antibodies were polyreactive and frequently bound to host or bacterial antigens. In one large clonal lineage of gp41-reactive antibodies, reactivity to HIV-1 Env was acquired only after somatic mutations. Polyreactive gp41-binding antibodies were also isolated from uninfected individuals. These data suggest that the majority of gp41-binding antibodies produced after acute HIV-1 infection are cross-reactive responses generated by stimulating memory B cells that have previously been activated by non–HIV-1 antigens.

Publisher

Rockefeller University Press

Subject

Immunology,Immunology and Allergy

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