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Design and crystal structure of a native-like HIV-1 envelope trimer that engages multiple broadly neutralizing antibody precursors in vivo

Design and crystal structure of a native-like HIV-1 envelope trimer that engages multiple broadly neutralizing antibody precursors in vivo
Design and crystal structure of a native-like HIV-1 envelope trimer that engages multiple broadly neutralizing antibody precursors in vivo

Induction of broadly neutralizing antibodies (bNAbs) by HIV-1 envelope glycoprotein immunogens would be a major advance toward an effective vaccine. A critical step in this process is the activation of naive B cells expressing germline (gl) antibody precursors that have the potential to evolve into bNAbs. Here, we reengineered the BG505 SOS IP.664 glycoprotein to engage gl precursors of bNAbs that target either the trimer apex or the CD4-binding site. The resulting BG505 SOS IP.v4.1- GT1 trimer binds multiple bNAb gl precursors in vitro. Immunization experiments in knock-in mice expressing gl-VRC01 or gl-PGT121 show that this trimer activates B cells in vivo, resulting in the secretion of specific antibodies into the sera. A crystal structure of the gl-targeting trimer at 3.2-Å resolution in complex with neutralizing antibodies 35O22 and 9H+109L reveals a native-like conformation and the successful incorporation of design features associated with binding of multiple gl-bNAb precursors.

0022-1007
2573-2590
Medina-Ramírez, Max
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Garces, Fernando
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Escolano, Amelia
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Skog, Patrick
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de Taeye, Steven W.
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Del Moral-Sanchez, Ivan
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McGuire, Andrew T.
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Yasmeen, Anila
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Behrens, Anna Janina
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Ozorowski, Gabriel
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van den Kerkhof, Tom L.G.M.
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Freund, Natalia T.
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Dosenovic, Pia
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Hua, Yuanzi
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Gitlin, Alexander D.
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Cupo, Albert
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van der Woude, Patricia
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Golabek, Michael
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Sliepen, Kwinten
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Blane, Tanya
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Kootstra, Neeltje
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van Breemen, Mariëlle J.
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Pritchard, Laura K.
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Stanfield, Robyn L.
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Crispin, Max
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Ward, Andrew B.
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Stamatatos, Leonidas
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Klasse, Per Johan
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Moore, John P.
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Nemazee, David
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Nussenzweig, Michel C.
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Wilson, Ian A.
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Sanders, Rogier W.
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Medina-Ramírez, Max
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Garces, Fernando
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Escolano, Amelia
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Skog, Patrick
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de Taeye, Steven W.
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Del Moral-Sanchez, Ivan
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McGuire, Andrew T.
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Yasmeen, Anila
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Behrens, Anna Janina
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Ozorowski, Gabriel
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van den Kerkhof, Tom L.G.M.
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Freund, Natalia T.
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Dosenovic, Pia
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Hua, Yuanzi
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Gitlin, Alexander D.
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Cupo, Albert
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van der Woude, Patricia
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Golabek, Michael
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Sliepen, Kwinten
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Blane, Tanya
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Kootstra, Neeltje
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van Breemen, Mariëlle J.
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Pritchard, Laura K.
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Stanfield, Robyn L.
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Crispin, Max
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Ward, Andrew B.
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Stamatatos, Leonidas
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Klasse, Per Johan
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Moore, John P.
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Nemazee, David
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Nussenzweig, Michel C.
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Wilson, Ian A.
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Sanders, Rogier W.
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Medina-Ramírez, Max, Garces, Fernando, Escolano, Amelia, Skog, Patrick, de Taeye, Steven W., Del Moral-Sanchez, Ivan, McGuire, Andrew T., Yasmeen, Anila, Behrens, Anna Janina, Ozorowski, Gabriel, van den Kerkhof, Tom L.G.M., Freund, Natalia T., Dosenovic, Pia, Hua, Yuanzi, Gitlin, Alexander D., Cupo, Albert, van der Woude, Patricia, Golabek, Michael, Sliepen, Kwinten, Blane, Tanya, Kootstra, Neeltje, van Breemen, Mariëlle J., Pritchard, Laura K., Stanfield, Robyn L., Crispin, Max, Ward, Andrew B., Stamatatos, Leonidas, Klasse, Per Johan, Moore, John P., Nemazee, David, Nussenzweig, Michel C., Wilson, Ian A. and Sanders, Rogier W. (2017) Design and crystal structure of a native-like HIV-1 envelope trimer that engages multiple broadly neutralizing antibody precursors in vivo. Journal of Experimental Medicine, 214 (9), 2573-2590. (doi:10.1084/jem.20161160).

Record type: Article

Abstract

Induction of broadly neutralizing antibodies (bNAbs) by HIV-1 envelope glycoprotein immunogens would be a major advance toward an effective vaccine. A critical step in this process is the activation of naive B cells expressing germline (gl) antibody precursors that have the potential to evolve into bNAbs. Here, we reengineered the BG505 SOS IP.664 glycoprotein to engage gl precursors of bNAbs that target either the trimer apex or the CD4-binding site. The resulting BG505 SOS IP.v4.1- GT1 trimer binds multiple bNAb gl precursors in vitro. Immunization experiments in knock-in mice expressing gl-VRC01 or gl-PGT121 show that this trimer activates B cells in vivo, resulting in the secretion of specific antibodies into the sera. A crystal structure of the gl-targeting trimer at 3.2-Å resolution in complex with neutralizing antibodies 35O22 and 9H+109L reveals a native-like conformation and the successful incorporation of design features associated with binding of multiple gl-bNAb precursors.

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Sanders JEM paper_2017
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More information

Accepted/In Press date: 12 May 2017
e-pub ahead of print date: 28 August 2017
Published date: 4 September 2017

Identifiers

Local EPrints ID: 414337
URI: http://eprints.soton.ac.uk/id/eprint/414337
ISSN: 0022-1007
PURE UUID: 10b78e19-803b-423b-bc2b-b0a6a1514acb
ORCID for Max Crispin: ORCID iD orcid.org/0000-0002-1072-2694

Catalogue record

Date deposited: 26 Sep 2017 16:30
Last modified: 11 Jul 2024 01:58

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Contributors

Author: Max Medina-Ramírez
Author: Fernando Garces
Author: Amelia Escolano
Author: Patrick Skog
Author: Steven W. de Taeye
Author: Ivan Del Moral-Sanchez
Author: Andrew T. McGuire
Author: Anila Yasmeen
Author: Anna Janina Behrens
Author: Gabriel Ozorowski
Author: Tom L.G.M. van den Kerkhof
Author: Natalia T. Freund
Author: Pia Dosenovic
Author: Yuanzi Hua
Author: Alexander D. Gitlin
Author: Albert Cupo
Author: Patricia van der Woude
Author: Michael Golabek
Author: Kwinten Sliepen
Author: Tanya Blane
Author: Neeltje Kootstra
Author: Mariëlle J. van Breemen
Author: Laura K. Pritchard
Author: Robyn L. Stanfield
Author: Max Crispin ORCID iD
Author: Andrew B. Ward
Author: Leonidas Stamatatos
Author: Per Johan Klasse
Author: John P. Moore
Author: David Nemazee
Author: Michel C. Nussenzweig
Author: Ian A. Wilson
Author: Rogier W. Sanders

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