By Binding CD80 and CD86, the Vaccinia Virus M2 Protein Blocks Their Interactions with both CD28 and CTLA4 and Potentiates CD80 Binding to PD-L1

In this article we report that the M2 protein encoded by the vaccinia virus is secreted as a homo-oligomer by infected cells and binds two central costimulation molecules, CD80 (B7-1) and CD86 (B7-2). These interactions block the ligation of the two B7 proteins to both soluble CD28 and soluble cytot...

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Autores principales: Kleinpeter, Patricia, Remy-Ziller, Christelle, Winter, Eline, Gantzer, Murielle, Nourtier, Virginie, Kempf, Juliette, Hortelano, Julie, Schmitt, Doris, Schultz, Huguette, Geist, Michel, Brua, Catherine, Hoffmann, Chantal, Schlesinger, Yasmin, Villeval, Dominique, Thioudellet, Christine, Erbs, Philippe, Foloppe, Johann, Silvestre, Nathalie, Fend, Laetitia, Quemeneur, Eric, Marchand, Jean-Baptiste
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Society for Microbiology 2019
Materias:
Virus-Cell Interactions
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6532080/
https://www.ncbi.nlm.nih.gov/pubmed/30918073
http://dx.doi.org/10.1128/JVI.00207-19
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author Kleinpeter, Patricia
Remy-Ziller, Christelle
Winter, Eline
Gantzer, Murielle
Nourtier, Virginie
Kempf, Juliette
Hortelano, Julie
Schmitt, Doris
Schultz, Huguette
Geist, Michel
Brua, Catherine
Hoffmann, Chantal
Schlesinger, Yasmin
Villeval, Dominique
Thioudellet, Christine
Erbs, Philippe
Foloppe, Johann
Silvestre, Nathalie
Fend, Laetitia
Quemeneur, Eric
Marchand, Jean-Baptiste
author_facet Kleinpeter, Patricia
Remy-Ziller, Christelle
Winter, Eline
Gantzer, Murielle
Nourtier, Virginie
Kempf, Juliette
Hortelano, Julie
Schmitt, Doris
Schultz, Huguette
Geist, Michel
Brua, Catherine
Hoffmann, Chantal
Schlesinger, Yasmin
Villeval, Dominique
Thioudellet, Christine
Erbs, Philippe
Foloppe, Johann
Silvestre, Nathalie
Fend, Laetitia
Quemeneur, Eric
Marchand, Jean-Baptiste
author_sort Kleinpeter, Patricia
collection PubMed
description In this article we report that the M2 protein encoded by the vaccinia virus is secreted as a homo-oligomer by infected cells and binds two central costimulation molecules, CD80 (B7-1) and CD86 (B7-2). These interactions block the ligation of the two B7 proteins to both soluble CD28 and soluble cytotoxic T-lymphocyte associated protein 4 (CTLA4) but favor the binding of soluble PD-L1 to soluble CD80. M2L gene orthologues are found in several other poxviruses, and the B7-CD28/CTLA4 blocking activity has been identified for several culture supernatants of orthopoxvirus-infected cells and for a recombinant myxoma virus M2 protein homolog (i.e., Gp120-like protein, or Gp120LP). Overall, these data indicate that the M2 poxvirus family of proteins may be involved in immunosuppressive activities broader than the NF-κB inhibition already reported (R. Gedey, X. L. Jin, O. Hinthong, and J. L. Shisler, J Virol 80:8676–8685, 2006, https://doi.org/10.1128/JVI.00935-06). A Copenhagen vaccinia virus with a deletion of the nonessential M2L locus was generated and compared with its parental virus. This M2L-deleted vaccinia virus, unlike the parental virus, does not generate interference with the B7-CD28/CTLA4/PD-L1 interactions. Moreover, this deletion did not affect any key features of the virus (in vitro replication, oncolytic activities in vitro and in vivo, and intratumoral expression of a transgene in an immunocompetent murine model). Altogether, these first results suggest that the M2 protein has the potential to be used as a new immunosuppressive biotherapeutic and that the M2L-deleted vaccinia virus represents an attractive new oncolytic platform with an improved immunological profile. IMPORTANCE The vaccinia virus harbors in its genome several genes dedicated to the inhibition of the host immune response. Among them, M2L was reported to inhibit the intracellular NF-κB pathway. We report here several new putative immunosuppressive activities of M2 protein. M2 protein is secreted and binds cornerstone costimulatory molecules (CD80/CD86). M2 binding to CD80/CD86 blocks their interaction with soluble CD28/CTLA4 but also favors the soluble PD-L1-CD80 association. These findings open the way for new investigations deciphering the immune system effects of soluble M2 protein. Moreover, a vaccinia virus with a deletion of its M2L has been generated and characterized as a new oncolytic platform. The replication and oncolytic activities of the M2L-deleted vaccinia virus are indistinguishable from those of the parental virus. More investigations are needed to characterize in detail the immune response triggered against both the tumor and the virus by this M2-defective vaccinia virus.
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spelling pubmed-65320802019-06-03 By Binding CD80 and CD86, the Vaccinia Virus M2 Protein Blocks Their Interactions with both CD28 and CTLA4 and Potentiates CD80 Binding to PD-L1 Kleinpeter, Patricia Remy-Ziller, Christelle Winter, Eline Gantzer, Murielle Nourtier, Virginie Kempf, Juliette Hortelano, Julie Schmitt, Doris Schultz, Huguette Geist, Michel Brua, Catherine Hoffmann, Chantal Schlesinger, Yasmin Villeval, Dominique Thioudellet, Christine Erbs, Philippe Foloppe, Johann Silvestre, Nathalie Fend, Laetitia Quemeneur, Eric Marchand, Jean-Baptiste J Virol Virus-Cell Interactions In this article we report that the M2 protein encoded by the vaccinia virus is secreted as a homo-oligomer by infected cells and binds two central costimulation molecules, CD80 (B7-1) and CD86 (B7-2). These interactions block the ligation of the two B7 proteins to both soluble CD28 and soluble cytotoxic T-lymphocyte associated protein 4 (CTLA4) but favor the binding of soluble PD-L1 to soluble CD80. M2L gene orthologues are found in several other poxviruses, and the B7-CD28/CTLA4 blocking activity has been identified for several culture supernatants of orthopoxvirus-infected cells and for a recombinant myxoma virus M2 protein homolog (i.e., Gp120-like protein, or Gp120LP). Overall, these data indicate that the M2 poxvirus family of proteins may be involved in immunosuppressive activities broader than the NF-κB inhibition already reported (R. Gedey, X. L. Jin, O. Hinthong, and J. L. Shisler, J Virol 80:8676–8685, 2006, https://doi.org/10.1128/JVI.00935-06). A Copenhagen vaccinia virus with a deletion of the nonessential M2L locus was generated and compared with its parental virus. This M2L-deleted vaccinia virus, unlike the parental virus, does not generate interference with the B7-CD28/CTLA4/PD-L1 interactions. Moreover, this deletion did not affect any key features of the virus (in vitro replication, oncolytic activities in vitro and in vivo, and intratumoral expression of a transgene in an immunocompetent murine model). Altogether, these first results suggest that the M2 protein has the potential to be used as a new immunosuppressive biotherapeutic and that the M2L-deleted vaccinia virus represents an attractive new oncolytic platform with an improved immunological profile. IMPORTANCE The vaccinia virus harbors in its genome several genes dedicated to the inhibition of the host immune response. Among them, M2L was reported to inhibit the intracellular NF-κB pathway. We report here several new putative immunosuppressive activities of M2 protein. M2 protein is secreted and binds cornerstone costimulatory molecules (CD80/CD86). M2 binding to CD80/CD86 blocks their interaction with soluble CD28/CTLA4 but also favors the soluble PD-L1-CD80 association. These findings open the way for new investigations deciphering the immune system effects of soluble M2 protein. Moreover, a vaccinia virus with a deletion of its M2L has been generated and characterized as a new oncolytic platform. The replication and oncolytic activities of the M2L-deleted vaccinia virus are indistinguishable from those of the parental virus. More investigations are needed to characterize in detail the immune response triggered against both the tumor and the virus by this M2-defective vaccinia virus. American Society for Microbiology 2019-05-15 /pmc/articles/PMC6532080/ /pubmed/30918073 http://dx.doi.org/10.1128/JVI.00207-19 Text en Copyright © 2019 Kleinpeter et al. https://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution 4.0 International license (https://creativecommons.org/licenses/by/4.0/) .
spellingShingle Virus-Cell Interactions
Kleinpeter, Patricia
Remy-Ziller, Christelle
Winter, Eline
Gantzer, Murielle
Nourtier, Virginie
Kempf, Juliette
Hortelano, Julie
Schmitt, Doris
Schultz, Huguette
Geist, Michel
Brua, Catherine
Hoffmann, Chantal
Schlesinger, Yasmin
Villeval, Dominique
Thioudellet, Christine
Erbs, Philippe
Foloppe, Johann
Silvestre, Nathalie
Fend, Laetitia
Quemeneur, Eric
Marchand, Jean-Baptiste
By Binding CD80 and CD86, the Vaccinia Virus M2 Protein Blocks Their Interactions with both CD28 and CTLA4 and Potentiates CD80 Binding to PD-L1
title By Binding CD80 and CD86, the Vaccinia Virus M2 Protein Blocks Their Interactions with both CD28 and CTLA4 and Potentiates CD80 Binding to PD-L1
title_full By Binding CD80 and CD86, the Vaccinia Virus M2 Protein Blocks Their Interactions with both CD28 and CTLA4 and Potentiates CD80 Binding to PD-L1
title_fullStr By Binding CD80 and CD86, the Vaccinia Virus M2 Protein Blocks Their Interactions with both CD28 and CTLA4 and Potentiates CD80 Binding to PD-L1
title_full_unstemmed By Binding CD80 and CD86, the Vaccinia Virus M2 Protein Blocks Their Interactions with both CD28 and CTLA4 and Potentiates CD80 Binding to PD-L1
title_short By Binding CD80 and CD86, the Vaccinia Virus M2 Protein Blocks Their Interactions with both CD28 and CTLA4 and Potentiates CD80 Binding to PD-L1
title_sort by binding cd80 and cd86, the vaccinia virus m2 protein blocks their interactions with both cd28 and ctla4 and potentiates cd80 binding to pd-l1
topic Virus-Cell Interactions
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6532080/
https://www.ncbi.nlm.nih.gov/pubmed/30918073
http://dx.doi.org/10.1128/JVI.00207-19
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