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Published April 8, 2013 | Supplemental Material + Published
Journal Article Open

Engineering HIV envelope protein to activate germline B cell receptors of broadly neutralizing anti-CD4 binding site antibodies

McGuire, Andrew T.
Hoot, Sam
Dreyer, Anita M.
Lippy, Adriana
Stuart, Andrew
Cohen, Kristen W.
Jardine, Joseph
Menis, Sergey
Scheid, Johannes F.
West, Anthony P.
Schief, William R.
Stamatatos, Leonidas

Abstract

Broadly neutralizing antibodies (bnAbs) against HIV are believed to be a critical component of the protective responses elicited by an effective HIV vaccine. Neutralizing antibodies against the evolutionarily conserved CD4-binding site (CD4-BS) on the HIV envelope glycoprotein (Env) are capable of inhibiting infection of diverse HIV strains, and have been isolated from HIV-infected individuals. Despite the presence of anti–CD4-BS broadly neutralizing antibody (bnAb) epitopes on recombinant Env, Env immunization has so far failed to elicit such antibodies. Here, we show that Env immunogens fail to engage the germline-reverted forms of known bnAbs that target the CD4-BS. However, we found that the elimination of a conserved glycosylation site located in Loop D and two glycosylation sites located in variable region 5 of Env allows Env-binding to, and activation of, B cells expressing the germline-reverted BCRs of two potent broadly neutralizing antibodies, VRC01 and NIH45-46. Our results offer a possible explanation as to why Env immunogens have been ineffective in stimulating the production of such bNAbs. Importantly, they provide key information as to how such immunogens can be engineered to initiate the process of antibody-affinity maturation against one of the most conserved Env regions.

Additional Information

© 2013 McGuire et al. This article is distributed under the terms of an Attribution–Noncommercial–Share Alike–No Mirror Sites license for the first six months after the publication date (see http://www.rupress.org/terms). After six months it is available under a Creative Commons License (Attribution–Noncommercial–Share Alike 3.0 Unported license, as described at http://creativecommons.org/licenses/by-nc-sa/3.0/). Submitted: 20 December 2012. Accepted: 5 March 2013. We thank Zachary Caldwell, Sara Carbonetti, Anna Gazumyan, Jolene Glenn, Sam Danziger, and D. Noah Sather for technical support. This work was supported by National Institute of Allergy and Infectious Diseases/HIV Vaccine Research and Design grant P01AI081625 and R56 AI047708 (L. Stamatatos). We also acknowledge support by the J.B Pendleton Charitable Trust and by the University of Washington Center for AIDS Research, an NIH funded program (P30 AI027757). A.M. Dreyer was supported by the Swiss National Science Foundation (PBBSP3 144245). The authors declare no competing financial interests.

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Published - J_Exp_Med-2013-McGuire-655-63.pdf

Supplemental Material - JEM_20122824_sm.pdf

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