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Conformational and Structural Features of HIV-1 gp120 Underlying the Dual Receptor Antagonism by Cross-Reactive Neutralizing Antibody m18

  1. Author:
    Gift, S. K.
    Zentner, I. J.
    Schon, A.
    McFadden, K.
    Umashankara, M.
    Rajagopal, S.
    Contarino, M.
    Duffy, C.
    Courter, J. R.
    Zhang, M. Y.
    Gershoni, J. M.
    Cocklin, S.
    Dimitrov, D. S.
    Smith, A. B.
    Freire, E.
    Chaiken, I. M.

  2. Author Address

    [Gift, Syna Kuriakose; Zentner, Isaac J.; McFadden, Karyn; Umashankara, M.; Rajagopal, Srivats; Contarino, Mark; Duffy, Caitlin; Cocklin, Simon; Chaiken, Irwin M.] Drexel Univ, Coll Med, Dept Biochem & Mol Biol, Philadelphia, PA 19102 USA. [Gift, Syna Kuriakose; Zentner, Isaac J.; McFadden, Karyn; Chaiken, Irwin M.] Drexel Univ, Coll Med, Biochem Grad Program, Philadelphia, PA 19102 USA. [Schoen, Arne; Freire, Ernesto] Johns Hopkins Univ, Dept Biol, Baltimore, MD 21218 USA. [Courter, Joel R.; Smith, Amos B., III] Univ Penn, Dept Chem, Philadelphia, PA 19104 USA. [Zhang, Mei-Yun] Univ Hong Kong, Dept Microbiol, AIDS Inst, Hong Kong, Hong Kong, Peoples R China. [Gershoni, Jonathan M.] Tel Aviv Univ, IL-69978 Tel Aviv, Israel. [Dimitrov, Dimiter S.] NCI, Ctr Canc Res Nanobiol Program, Ctr Canc Res, NIH, Frederick, MD 21702 USA.;Chaiken, IM, Drexel Univ, Coll Med, Dept Biochem & Mol Biol, 11102 New Coll Bldg,MS 497,245N 15th St, Philadelphia, PA 19102 USA.;ichaiken@drexelmed.edu
    1. Year: 2011
    2. Date: Apr
  2. Journal: Biochemistry
    1. 50
    2. 14
    3. Pages: 2756-2768
  4. Type of Article: Article
  5. ISSN: 0006-2960
  1. Abstract:

    We investigated the interaction between cross-reactive HIV-1 neutralizing human monoclonal antibody m18 and HIV-IYU-2 gp120 in an effort to understand how this antibody inhibits the entry of virus into cells. m18 binds to gp120 with high affinity (K-D approximate to 5 nM) as measured by surface plasmon resonance (SPR) and isothermal titration calorimetry (ITC). SPR analysis further showed that m18 inhibits interactions of gp120 with both soluble CD4 and CD4-induced antibodies that have epitopes overlapping the coreceptor binding site. This dual receptor site antagonism, which occurs with equal potency for both inhibition effects, argues that m18 is not functioning as a mimic of CD4, in spite of the presence of a putative CD4-like loop formed by HCDR3 in the antibody. Consistent with this view, m18 was found to interact with gp120 in the presence of saturating concentrations of a CD4-mimicking small molecule gp120 inhibitor, suggesting that m18 does not require unoccupied CD4 Pbe43 binding cavity residues of gp120. Thermodynamic analysis of the m18 gp120 interaction suggests that m18 stabilizes a conformation of gp120 that is unique from and less structured than the CD4-stabilized conformation. Conformational mutants of gp120 were studied for their impact on m18 interaction. Mutations known to disrupt the coreceptor binding region and to lead to complete suppression of 17b binding had minimal effects on m18 binding. This argues that energetically important epitopes for m18 binding lie outside the disrupted bridging sheet region used for 17b and coreceptor binding. In contrast, mutations in the CD4 region strongly affected m18 binding. Overall, the results obtained in this work argue that m18, rather than mimicking CD4 directly, suppresses both receptor binding site functions of HIV-1 gp120 by stabilizing a nonproductive conformation of the envelope protein. These results can be related to prior findings about the importance of conformational entrapment as a common mode of action for neutralizing CD4bs antibodies, with differences mainly in epitope utilization and the extent of gp120 structuring.

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External Sources

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  2. DOI: 10.1021/bi101160r
  3. View record in Web of ScienceĀ®
  4. WOS: 000289029200007

Library Notes

  1. Fiscal Year: FY2010-2011
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