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Neutralizing antibodies induced by first-generation gp41-stabilized HIV-1 envelope trimers and nanoparticles

Neutralizing antibodies induced by first-generation gp41-stabilized HIV-1 envelope trimers and nanoparticles
Neutralizing antibodies induced by first-generation gp41-stabilized HIV-1 envelope trimers and nanoparticles

The immunogenicity of gp41-stabilized HIV-1 BG505 envelope (Env) trimers and nanoparticles (NPs) was recently assessed in mice and rabbits. Here, we combined Env-specific B-cell sorting and repertoire sequencing to identify neutralizing antibodies (NAbs) from immunized animals. A panel of mouse NAbs was isolated from mice immunized with a 60-meric I3-01 NP presenting 20 stabilized trimers. Three mouse NAbs potently neutralized BG505.T332N by recognizing a glycan epitope centered in the C3/V4 region on BG505 Env, as revealed by electron microscopy (EM), X-ray crystallography, and epitope mapping. A set of rabbit NAbs was isolated from rabbits immunized with a soluble trimer and a 24-meric ferritin NP presenting 8 trimers. Neutralization assays against BG505.T332N variants confirmed that potent rabbit NAbs targeted previously described glycan holes on BG505 Env and accounted for a significant portion of the autologous NAb response in both the trimer and ferritin NP groups. Last, we examined NAb responses that were induced by non-BG505 Env immunogens. We determined a 3.4-Å-resolution crystal structure for the clade C transmitted/founder (T/F) Du172.17 Env with a redesigned heptad repeat 1 (HR1) bend in gp41. This clade C Env, in a soluble trimer form and in a multivalent form with 8 trimers attached to ferritin NP, and the gp41-stabilized clade A Q482-d12 Env trimer elicited distinct NAb responses in rabbits, with notable differences in neutralization breadth. Although eliciting a broad NAb response remains a major challenge, our study provides valuable information on an HIV-1 vaccine design strategy that combines gp41 stabilization and NP display. IMPORTANCE Self-assembling protein nanoparticles (NPs) presenting BG505 envelope (Env) trimers can elicit tier 2 HIV-1-neutralizing antibody (NAb) responses more effectively than soluble trimers. In the present study, monoclonal NAbs were isolated from previously immunized mice and rabbits for structural and functional analyses, which revealed that potent mouse NAbs recognize the C3/V4 region and small NP-elicited rabbit NAbs primarily target known glycan holes on BG505 Env. This study validates the gp41 stabilization strategy for HIV-1 Env vaccine design and highlights the challenge in eliciting a broad NAb response.

HIV-1 vaccine design, envelope trimer, glycan holes, gp41 stabilization, nanoparticle, neutralizing antibodies
2150-7511
e0042921
Kumar, Sonu
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Lin, Xiaohe
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Ngo, Timothy
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Shapero, Benjamin
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Sou, Cindy
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Allen, Joel D
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Copps, Jeffrey
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Zhang, Lei
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Ozorowski, Gabriel
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He, Linling
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Crispin, Max
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Ward, Andrew B
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Wilson, Ian A
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Zhu, Jiang
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Kumar, Sonu
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Lin, Xiaohe
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Ngo, Timothy
f498a6f8-cd29-4f5f-b819-40fe4e7274c9
Shapero, Benjamin
31ddfcdc-a2bd-4c34-96b2-75237ed3cebc
Sou, Cindy
5340df80-f4b0-4a3b-b17a-4bb1d7194f6a
Allen, Joel D
c89d5569-7659-4835-b535-c9586e956b3a
Copps, Jeffrey
05d24804-b883-4b53-b688-f27f4f55c076
Zhang, Lei
e9a272bb-6497-4a84-baf9-425361f20830
Ozorowski, Gabriel
9d448a80-7310-4b30-ba44-ee8b18222a02
He, Linling
c873e7ef-37de-4629-b646-19e06d13e38f
Crispin, Max
cd980957-0943-4b89-b2b2-710f01f33bc9
Ward, Andrew B
7b743524-72d4-448d-b645-11c55782b656
Wilson, Ian A
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Zhu, Jiang
ac20c27b-89fb-4ede-8cf8-c6f55270eacd

Kumar, Sonu, Lin, Xiaohe, Ngo, Timothy, Shapero, Benjamin, Sou, Cindy, Allen, Joel D, Copps, Jeffrey, Zhang, Lei, Ozorowski, Gabriel, He, Linling, Crispin, Max, Ward, Andrew B, Wilson, Ian A and Zhu, Jiang (2021) Neutralizing antibodies induced by first-generation gp41-stabilized HIV-1 envelope trimers and nanoparticles. mBio, 12 (3), e0042921, [e00429-21]. (doi:10.1128/mBio.00429-21).

Record type: Article

Abstract

The immunogenicity of gp41-stabilized HIV-1 BG505 envelope (Env) trimers and nanoparticles (NPs) was recently assessed in mice and rabbits. Here, we combined Env-specific B-cell sorting and repertoire sequencing to identify neutralizing antibodies (NAbs) from immunized animals. A panel of mouse NAbs was isolated from mice immunized with a 60-meric I3-01 NP presenting 20 stabilized trimers. Three mouse NAbs potently neutralized BG505.T332N by recognizing a glycan epitope centered in the C3/V4 region on BG505 Env, as revealed by electron microscopy (EM), X-ray crystallography, and epitope mapping. A set of rabbit NAbs was isolated from rabbits immunized with a soluble trimer and a 24-meric ferritin NP presenting 8 trimers. Neutralization assays against BG505.T332N variants confirmed that potent rabbit NAbs targeted previously described glycan holes on BG505 Env and accounted for a significant portion of the autologous NAb response in both the trimer and ferritin NP groups. Last, we examined NAb responses that were induced by non-BG505 Env immunogens. We determined a 3.4-Å-resolution crystal structure for the clade C transmitted/founder (T/F) Du172.17 Env with a redesigned heptad repeat 1 (HR1) bend in gp41. This clade C Env, in a soluble trimer form and in a multivalent form with 8 trimers attached to ferritin NP, and the gp41-stabilized clade A Q482-d12 Env trimer elicited distinct NAb responses in rabbits, with notable differences in neutralization breadth. Although eliciting a broad NAb response remains a major challenge, our study provides valuable information on an HIV-1 vaccine design strategy that combines gp41 stabilization and NP display. IMPORTANCE Self-assembling protein nanoparticles (NPs) presenting BG505 envelope (Env) trimers can elicit tier 2 HIV-1-neutralizing antibody (NAb) responses more effectively than soluble trimers. In the present study, monoclonal NAbs were isolated from previously immunized mice and rabbits for structural and functional analyses, which revealed that potent mouse NAbs recognize the C3/V4 region and small NP-elicited rabbit NAbs primarily target known glycan holes on BG505 Env. This study validates the gp41 stabilization strategy for HIV-1 Env vaccine design and highlights the challenge in eliciting a broad NAb response.

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Published date: 29 June 2021
Additional Information: Funding Information: Use of the APS was supported by the DOE, Basic Energy Sciences, Office of Science, under contract no. DE-AC02-06CH11357. Use of the SSRL was supported by the U.S. Department of Energy, Basic Energy Sciences, Office of Science, under contract no. DE-AC02-76SF00515. This work was supported by the International AIDS Vaccine Initiative (IAVI) through grant INV-008352/OPP1153692 (M.C.) and the IAVI Neutralizing Antibody Center through the Collaboration for AIDS Vaccine Discovery grants OPP1196345/INV-008813 (I.A.W., A.B.W., and M.C.), funded by the Bill and Melinda Gates Foundation; Scripps Consortium for HIV/AIDS Vaccine Development (CHAVD 1UM1 AI144462) (M.C., A.B.W., and I.A.W.); HIV Vaccine Research and Design (HIVRAD) program (P01 AI124337) (J.Z.); and NIH grants R01 AI129698 (J.Z.) and R01 AI140844 (J.Z.). Publisher Copyright: © 2021, American Society for Microbiology. All rights reserved.
Keywords: HIV-1 vaccine design, envelope trimer, glycan holes, gp41 stabilization, nanoparticle, neutralizing antibodies

Identifiers

Local EPrints ID: 450394
URI: http://eprints.soton.ac.uk/id/eprint/450394
ISSN: 2150-7511
PURE UUID: 38f6f21d-a31c-48aa-8383-ef81c8bf713d
ORCID for Joel D Allen: ORCID iD orcid.org/0000-0003-2547-968X
ORCID for Max Crispin: ORCID iD orcid.org/0000-0002-1072-2694

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Date deposited: 27 Jul 2021 17:23
Last modified: 17 Mar 2024 04:09

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Contributors

Author: Sonu Kumar
Author: Xiaohe Lin
Author: Timothy Ngo
Author: Benjamin Shapero
Author: Cindy Sou
Author: Joel D Allen ORCID iD
Author: Jeffrey Copps
Author: Lei Zhang
Author: Gabriel Ozorowski
Author: Linling He
Author: Max Crispin ORCID iD
Author: Andrew B Ward
Author: Ian A Wilson
Author: Jiang Zhu

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