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Published November 2019 | Published
Journal Article Open

Novel highly potent CD4bs bNAb with restricted pathway to HIV-1 escape

Schommers, P.
Gruell, H.
Abernathy, M. E.
Dingens, A. S.
Tran, M.-K.
Gristick, H. B. ORCID icon
Barnes, C. O. ORCID icon
Schoofs, T.
Schlotz, M.
Vanshylla, K.
Kreer, C.
Weiland, D.
Holtick, U.
Scheid, C.
Valter, M. M.
van Gils, M. J.
Sanders, R. W.
Vehreschild, J. J.
Cornely, O. A.
Lehmann, C.
Fätkenheuer, G.
Seaman, M. S.
Bloom, J. D. ORCID icon
Bjorkman, P. J. ORCID icon
Klein, F.

Abstract

Purpose: Broadly HIV-1 neutralizing antibodies (bNAbs) can suppress viremia in humans and represent a novel approach for effective immunotherapy. However, bNAb monotherapy selects for antibody-resistant viral variants. Thus, we focused on the identification of new antibody combinations and/or novel bNAbs that restrict pathways of HIV-1 escape. Methods: We screened HIV-1 positive patients for their neutralizing capacities. Following, we performed single cell sorting and PCR of HIV-1 Env-reactive mature B cells of identified elite neutralizers. Found antibodies were tested for neutralization and binding capacities in vitro. Further, their antiviral activity was tested in an HIV-1 infected humanized mouse model. Results: Here we report the isolation of antibody 1–18, a VH1–46-encoded CD4 binding site (CD4bs) bNAb identified in an individual ranking among the top 1% neutralizers of 2,274 HIV-1-infected subjects. Tested on a 119-virus panel, 1–18 showed to be exceptionally broad and potent with a coverage of 97% and a mean IC50 of 0.048 lg/mL, exceeding the activity of most potent CD4bs bNAbs described to-date. A 2.4 Å cryo-EM structure of 1–18 bound to a native-like Env trimer revealed that it interacts with HIV-1 env similar to other CD4bs bNAbs, but includes additional contacts to the V3 loop of the adjacent protomer. Notably, in vitro, 1–18 maintained activity against viruses carrying mutations associated with escape from VRC01-class bNAbs. Further, its HIV-1 env wide escape profile differed critically from other CD4bs bNAbs. In humanized mice, monotherapy with 1–18 was sufficient to prevent the development of viral escape variants that rapidly emerged during treatment with other CD4bs bNAbs. Finally, 1–18 overcame classical HIV-1 mutations that are driven by VRC01-like bNAbs in vivo. Conclusion: 1–18 is a highly potent and broad bNAb that restricts escape and overcomes frequent CD4bs escape pathways, providing new options for bNAb combinations to prevent and treat HIV-1 infection.

Additional Information

© 2019 The Authors. HIV Medicine © 2019 British HIV Association. First published: 06 November 2019.

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August 19, 2023
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