Two immunodominant domains of gp41 bind antibodies which enhance human immunodeficiency virus type 1 infection in vitro.

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J Virol. 1991 August; 65(8): 4169-4176

Two immunodominant domains of gp41 bind antibodies which enhance human immunodeficiency virus type 1 infection in vitro.

W E Robinson Jr, M K Gorny, J Y Xu, W M Mitchell and S Zolla-Pazner

Department of Pathology, Vanderbilt University, Nashville, Tennessee 37232-2561.

ABSTRACT

Four of eight human monoclonal antibodies (huMAbs) to gp41 wereidentified which could enhance human immunodeficiency virustype 1 (HIV-1) infection in vitro by complement-mediated antibody-dependentenhancement (C'-ADE). These enhancing huMAbs were mapped totwo distinct domains on the HIV-1 gp41 transmembrane glycoproteinby using synthetic peptides. The first domain, amino acids 579to 613 (peptide AA579-613), was recognized by three of the fourenhancing huMAbs. The AA579-613 peptide blocked C'-ADE of HIV-1infection in vitro whether it was mediated by these three huMAbsor by human polyclonal anti-HIV serum. The second domain, aminoacids 644 to 663, bound the remaining enhancing huMAb. Thispeptide weakly blocked C'-ADE mediated by the huMAb and by anHIV immune globulin fraction but did not block C'-ADE mediatedby a patient's serum. The patient's serum did react with thepeptide in an enzyme immunoassay. The huMAbs to the two domainscould interact in vitro to enhance HIV-1 infection in a synergisticmanner. These two domains, which bind enhancing antibodies,are conserved between HIV-1 isolates as well as between HIV-2and simian immunodeficiency virus isolates. These data demonstratethe existence of two conserved regions within the HIV-1 gp41which bind enhancing antibodies; these two domains, amino acids579 to 613 and 644 to 663, may prove important in HIV-1 vaccinedevelopment and in immunopathogenesis of HIV-1 infection.

J Virol. 1991 August; 65(8): 4169-4176

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