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. 2002 Dec 12;420(6916):678-82.
doi: 10.1038/nature01188.

HIV-1 evades antibody-mediated neutralization through conformational masking of receptor-binding sites

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HIV-1 evades antibody-mediated neutralization through conformational masking of receptor-binding sites

Peter D Kwong et al. Nature. .

Abstract

The ability of human immunodeficiency virus (HIV-1) to persist and cause AIDS is dependent on its avoidance of antibody-mediated neutralization. The virus elicits abundant, envelope-directed antibodies that have little neutralization capacity. This lack of neutralization is paradoxical, given the functional conservation and exposure of receptor-binding sites on the gp120 envelope glycoprotein, which are larger than the typical antibody footprint and should therefore be accessible for antibody binding. Because gp120-receptor interactions involve conformational reorganization, we measured the entropies of binding for 20 gp120-reactive antibodies. Here we show that recognition by receptor-binding-site antibodies induces conformational change. Correlation with neutralization potency and analysis of receptor-antibody thermodynamic cycles suggested a receptor-binding-site 'conformational masking' mechanism of neutralization escape. To understand how such an escape mechanism would be compatible with virus-receptor interactions, we tested a soluble dodecameric receptor molecule and found that it neutralized primary HIV-1 isolates with great potency, showing that simultaneous binding of viral envelope glycoproteins by multiple receptors creates sufficient avidity to compensate for such masking. Because this solution is available for cell-surface receptors but not for most antibodies, conformational masking enables HIV-1 to maintain receptor binding and simultaneously to resist neutralization.

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Comment in

  • HIV: conformational camouflage.
    Jardetzky T. Jardetzky T. Nature. 2002 Dec 12;420(6916):623-4. doi: 10.1038/420623a. Nature. 2002. PMID: 12478278 No abstract available.

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