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Polyclonal antibody responses to HIV Env immunogens resolved using cryoEM

Polyclonal antibody responses to HIV Env immunogens resolved using cryoEM
Polyclonal antibody responses to HIV Env immunogens resolved using cryoEM
Engineered ectodomain trimer immunogens based on BG505 envelope glycoprotein are widely utilized as components of HIV vaccine development platforms. In this study, we used rhesus macaques to evaluate the immunogenicity of several stabilized BG505 SOSIP constructs both as free trimers and presented on a nanoparticle. We applied a cryoEM-based method for high-resolution mapping of polyclonal antibody responses elicited in immunized animals (cryoEMPEM). Mutational analysis coupled with neutralization assays were used to probe the neutralization potential at each epitope. We demonstrate that cryoEMPEM data can be used for rapid, high-resolution analysis of polyclonal antibody responses without the need for monoclonal antibody isolation. This approach allowed to resolve structurally distinct classes of antibodies that bind overlapping sites. In addition to comprehensive mapping of commonly targeted neutralizing and non-neutralizing epitopes in BG505 SOSIP immunogens, our analysis revealed that epitopes comprising engineered stabilizing mutations and of partially occupied glycosylation sites can be immunogenic.
2041-1723
4817
Antanasijevic, Aleksandar
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Sewall, Leigh M
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Cottrell, Christopher A
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Carnathan, Diane G
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Jimenez, Luis E
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Ngo, Julia T
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Silverman, Jennifer B
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Groschel, Bettina
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Georgeson, Erik
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Bhiman, Jinal
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Bastidas, Raiza
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LaBranche, Celia
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Allen, Joel D
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Copps, Jeffrey
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Perrett, Hailee R
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Rantalainen, Kimmo
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Cannac, Fabien
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Yang, Yuhe R
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de la Peña, Alba Torrents
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Rocha, Rebeca Froes
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Berndsen, Zachary T
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King, Neil P
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Sanders, Rogier W
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Moore, John P
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Crotty, Shane
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Crispin, Max
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Montefiori, David C
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Burton, Dennis R
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Schief, William R
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Silvestri, Guido
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Ward, Andrew B
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Antanasijevic, Aleksandar
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Sewall, Leigh M
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Cottrell, Christopher A
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Carnathan, Diane G
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Jimenez, Luis E
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Ngo, Julia T
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Silverman, Jennifer B
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Groschel, Bettina
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Georgeson, Erik
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Bhiman, Jinal
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Bastidas, Raiza
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LaBranche, Celia
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Allen, Joel D
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Copps, Jeffrey
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Perrett, Hailee R
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Rantalainen, Kimmo
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Cannac, Fabien
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Yang, Yuhe R
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de la Peña, Alba Torrents
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Rocha, Rebeca Froes
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Berndsen, Zachary T
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King, Neil P
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Sanders, Rogier W
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Moore, John P
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Crotty, Shane
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Crispin, Max
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Montefiori, David C
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Burton, Dennis R
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Schief, William R
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Silvestri, Guido
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Ward, Andrew B
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Antanasijevic, Aleksandar, Sewall, Leigh M, Cottrell, Christopher A, Carnathan, Diane G, Jimenez, Luis E, Ngo, Julia T, Silverman, Jennifer B, Groschel, Bettina, Georgeson, Erik, Bhiman, Jinal, Bastidas, Raiza, LaBranche, Celia, Allen, Joel D, Copps, Jeffrey, Perrett, Hailee R, Rantalainen, Kimmo, Cannac, Fabien, Yang, Yuhe R, de la Peña, Alba Torrents, Rocha, Rebeca Froes, Berndsen, Zachary T, King, Neil P, Sanders, Rogier W, Moore, John P, Crotty, Shane, Crispin, Max, Montefiori, David C, Burton, Dennis R, Schief, William R, Silvestri, Guido and Ward, Andrew B (2021) Polyclonal antibody responses to HIV Env immunogens resolved using cryoEM. Nature Communications, 12 (1), 4817, [4817]. (doi:10.1038/s41467-021-25087-4).

Record type: Article

Abstract

Engineered ectodomain trimer immunogens based on BG505 envelope glycoprotein are widely utilized as components of HIV vaccine development platforms. In this study, we used rhesus macaques to evaluate the immunogenicity of several stabilized BG505 SOSIP constructs both as free trimers and presented on a nanoparticle. We applied a cryoEM-based method for high-resolution mapping of polyclonal antibody responses elicited in immunized animals (cryoEMPEM). Mutational analysis coupled with neutralization assays were used to probe the neutralization potential at each epitope. We demonstrate that cryoEMPEM data can be used for rapid, high-resolution analysis of polyclonal antibody responses without the need for monoclonal antibody isolation. This approach allowed to resolve structurally distinct classes of antibodies that bind overlapping sites. In addition to comprehensive mapping of commonly targeted neutralizing and non-neutralizing epitopes in BG505 SOSIP immunogens, our analysis revealed that epitopes comprising engineered stabilizing mutations and of partially occupied glycosylation sites can be immunogenic.

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Published article_Antanasijevic_Nat Comms_2021
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Accepted/In Press date: 23 July 2021
Published date: 10 August 2021

Identifiers

Local EPrints ID: 450899
URI: http://eprints.soton.ac.uk/id/eprint/450899
ISSN: 2041-1723
PURE UUID: a3fc8f2a-6150-4d2d-8e70-66f76d2f7bd4
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

Catalogue record

Date deposited: 19 Aug 2021 16:31
Last modified: 11 Jul 2024 02:10

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Contributors

Author: Aleksandar Antanasijevic
Author: Leigh M Sewall
Author: Christopher A Cottrell
Author: Diane G Carnathan
Author: Luis E Jimenez
Author: Julia T Ngo
Author: Jennifer B Silverman
Author: Bettina Groschel
Author: Erik Georgeson
Author: Jinal Bhiman
Author: Raiza Bastidas
Author: Celia LaBranche
Author: Joel D Allen ORCID iD
Author: Jeffrey Copps
Author: Hailee R Perrett
Author: Kimmo Rantalainen
Author: Fabien Cannac
Author: Yuhe R Yang
Author: Alba Torrents de la Peña
Author: Rebeca Froes Rocha
Author: Zachary T Berndsen
Author: Neil P King
Author: Rogier W Sanders
Author: John P Moore
Author: Shane Crotty
Author: Max Crispin ORCID iD
Author: David C Montefiori
Author: Dennis R Burton
Author: William R Schief
Author: Guido Silvestri
Author: Andrew B Ward

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