CCR5 structural plasticity shapes HIV-1 phenotypic properties

CCR5 plays immune functions and is the coreceptor for R5 HIV-1 strains. It exists in diverse conformations and oligomerization states. We interrogated the significance of the CCR5 structural diversity on HIV-1 infection. We show that envelope glycoproteins (gp120s) from different HIV-1 strains exhib...

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Autores principales: Colin, Philippe, Zhou, Zhicheng, Staropoli, Isabelle, Garcia-Perez, Javier, Gasser, Romain, Armani-Tourret, Marie, Benureau, Yann, Gonzalez, Nuria, Jin, Jun, Connell, Bridgette J., Raymond, Stéphanie, Delobel, Pierre, Izopet, Jacques, Lortat-Jacob, Hugues, Alcami, Jose, Arenzana-Seisdedos, Fernando, Brelot, Anne, Lagane, Bernard
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2018
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6283471/
https://www.ncbi.nlm.nih.gov/pubmed/30521629
http://dx.doi.org/10.1371/journal.ppat.1007432
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author Colin, Philippe
Zhou, Zhicheng
Staropoli, Isabelle
Garcia-Perez, Javier
Gasser, Romain
Armani-Tourret, Marie
Benureau, Yann
Gonzalez, Nuria
Jin, Jun
Connell, Bridgette J.
Raymond, Stéphanie
Delobel, Pierre
Izopet, Jacques
Lortat-Jacob, Hugues
Alcami, Jose
Arenzana-Seisdedos, Fernando
Brelot, Anne
Lagane, Bernard
author_facet Colin, Philippe
Zhou, Zhicheng
Staropoli, Isabelle
Garcia-Perez, Javier
Gasser, Romain
Armani-Tourret, Marie
Benureau, Yann
Gonzalez, Nuria
Jin, Jun
Connell, Bridgette J.
Raymond, Stéphanie
Delobel, Pierre
Izopet, Jacques
Lortat-Jacob, Hugues
Alcami, Jose
Arenzana-Seisdedos, Fernando
Brelot, Anne
Lagane, Bernard
author_sort Colin, Philippe
collection PubMed
description CCR5 plays immune functions and is the coreceptor for R5 HIV-1 strains. It exists in diverse conformations and oligomerization states. We interrogated the significance of the CCR5 structural diversity on HIV-1 infection. We show that envelope glycoproteins (gp120s) from different HIV-1 strains exhibit divergent binding levels to CCR5 on cell lines and primary cells, but not to CD4 or the CD4i monoclonal antibody E51. This owed to differential binding of the gp120s to different CCR5 populations, which exist in varying quantities at the cell surface and are differentially expressed between different cell types. Some, but not all, of these populations are antigenically distinct conformations of the coreceptor. The different binding levels of gp120s also correspond to differences in their capacity to bind CCR5 dimers/oligomers. Mutating the CCR5 dimerization interface changed conformation of the CCR5 homodimers and modulated differentially the binding of distinct gp120s. Env-pseudotyped viruses also use particular CCR5 conformations for entry, which may differ between different viruses and represent a subset of those binding gp120s. In particular, even if gp120s can bind both CCR5 monomers and oligomers, impairment of CCR5 oligomerization improved viral entry, suggesting that HIV-1 prefers monomers for entry. From a functional standpoint, we illustrate that the nature of the CCR5 molecules to which gp120/HIV-1 binds shapes sensitivity to inhibition by CCR5 ligands and cellular tropism. Differences exist in the CCR5 populations between T-cells and macrophages, and this is associated with differential capacity to bind gp120s and to support viral entry. In macrophages, CCR5 structural plasticity is critical for entry of blood-derived R5 isolates, which, in contrast to prototypical M-tropic strains from brain tissues, cannot benefit from enhanced affinity for CD4. Collectively, our results support a role for CCR5 heterogeneity in diversifying the phenotypic properties of HIV-1 isolates and provide new clues for development of CCR5-targeting drugs.
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spelling pubmed-62834712018-12-20 CCR5 structural plasticity shapes HIV-1 phenotypic properties Colin, Philippe Zhou, Zhicheng Staropoli, Isabelle Garcia-Perez, Javier Gasser, Romain Armani-Tourret, Marie Benureau, Yann Gonzalez, Nuria Jin, Jun Connell, Bridgette J. Raymond, Stéphanie Delobel, Pierre Izopet, Jacques Lortat-Jacob, Hugues Alcami, Jose Arenzana-Seisdedos, Fernando Brelot, Anne Lagane, Bernard PLoS Pathog Research Article CCR5 plays immune functions and is the coreceptor for R5 HIV-1 strains. It exists in diverse conformations and oligomerization states. We interrogated the significance of the CCR5 structural diversity on HIV-1 infection. We show that envelope glycoproteins (gp120s) from different HIV-1 strains exhibit divergent binding levels to CCR5 on cell lines and primary cells, but not to CD4 or the CD4i monoclonal antibody E51. This owed to differential binding of the gp120s to different CCR5 populations, which exist in varying quantities at the cell surface and are differentially expressed between different cell types. Some, but not all, of these populations are antigenically distinct conformations of the coreceptor. The different binding levels of gp120s also correspond to differences in their capacity to bind CCR5 dimers/oligomers. Mutating the CCR5 dimerization interface changed conformation of the CCR5 homodimers and modulated differentially the binding of distinct gp120s. Env-pseudotyped viruses also use particular CCR5 conformations for entry, which may differ between different viruses and represent a subset of those binding gp120s. In particular, even if gp120s can bind both CCR5 monomers and oligomers, impairment of CCR5 oligomerization improved viral entry, suggesting that HIV-1 prefers monomers for entry. From a functional standpoint, we illustrate that the nature of the CCR5 molecules to which gp120/HIV-1 binds shapes sensitivity to inhibition by CCR5 ligands and cellular tropism. Differences exist in the CCR5 populations between T-cells and macrophages, and this is associated with differential capacity to bind gp120s and to support viral entry. In macrophages, CCR5 structural plasticity is critical for entry of blood-derived R5 isolates, which, in contrast to prototypical M-tropic strains from brain tissues, cannot benefit from enhanced affinity for CD4. Collectively, our results support a role for CCR5 heterogeneity in diversifying the phenotypic properties of HIV-1 isolates and provide new clues for development of CCR5-targeting drugs. Public Library of Science 2018-12-06 /pmc/articles/PMC6283471/ /pubmed/30521629 http://dx.doi.org/10.1371/journal.ppat.1007432 Text en © 2018 Colin et al http://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Colin, Philippe
Zhou, Zhicheng
Staropoli, Isabelle
Garcia-Perez, Javier
Gasser, Romain
Armani-Tourret, Marie
Benureau, Yann
Gonzalez, Nuria
Jin, Jun
Connell, Bridgette J.
Raymond, Stéphanie
Delobel, Pierre
Izopet, Jacques
Lortat-Jacob, Hugues
Alcami, Jose
Arenzana-Seisdedos, Fernando
Brelot, Anne
Lagane, Bernard
CCR5 structural plasticity shapes HIV-1 phenotypic properties
title CCR5 structural plasticity shapes HIV-1 phenotypic properties
title_full CCR5 structural plasticity shapes HIV-1 phenotypic properties
title_fullStr CCR5 structural plasticity shapes HIV-1 phenotypic properties
title_full_unstemmed CCR5 structural plasticity shapes HIV-1 phenotypic properties
title_short CCR5 structural plasticity shapes HIV-1 phenotypic properties
title_sort ccr5 structural plasticity shapes hiv-1 phenotypic properties
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6283471/
https://www.ncbi.nlm.nih.gov/pubmed/30521629
http://dx.doi.org/10.1371/journal.ppat.1007432
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