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A Short Double-Stapled Peptide Inhibits Respiratory Syncytial Virus Entry and Spreading

Synthetic peptides derived from the heptad repeat (HR) of fusion (F) proteins can be used as dominant negative inhibitors to inhibit the fusion mechanism of class I viral F proteins. Here, we have performed a stapled-peptide scan across the HR2 domain of the respiratory syncytial virus (RSV) F prote...

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Autores principales: Gaillard, Vanessa, Galloux, Marie, Garcin, Dominique, Eléouët, Jean-François, Le Goffic, Ronan, Larcher, Thibaut, Rameix-Welti, Marie-Anne, Boukadiri, Abdelhak, Héritier, Julien, Segura, Jean-Manuel, Baechler, Elodie, Arrell, Miriam, Mottet-Osman, Geneviève, Nyanguile, Origène
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Society for Microbiology 2017
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5365662/
https://www.ncbi.nlm.nih.gov/pubmed/28137809
http://dx.doi.org/10.1128/AAC.02241-16
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author Gaillard, Vanessa
Galloux, Marie
Garcin, Dominique
Eléouët, Jean-François
Le Goffic, Ronan
Larcher, Thibaut
Rameix-Welti, Marie-Anne
Boukadiri, Abdelhak
Héritier, Julien
Segura, Jean-Manuel
Baechler, Elodie
Arrell, Miriam
Mottet-Osman, Geneviève
Nyanguile, Origène
author_facet Gaillard, Vanessa
Galloux, Marie
Garcin, Dominique
Eléouët, Jean-François
Le Goffic, Ronan
Larcher, Thibaut
Rameix-Welti, Marie-Anne
Boukadiri, Abdelhak
Héritier, Julien
Segura, Jean-Manuel
Baechler, Elodie
Arrell, Miriam
Mottet-Osman, Geneviève
Nyanguile, Origène
author_sort Gaillard, Vanessa
collection PubMed
description Synthetic peptides derived from the heptad repeat (HR) of fusion (F) proteins can be used as dominant negative inhibitors to inhibit the fusion mechanism of class I viral F proteins. Here, we have performed a stapled-peptide scan across the HR2 domain of the respiratory syncytial virus (RSV) F protein with the aim to identify a minimal domain capable of disrupting the formation of the postfusion six-helix bundle required for viral cell entry. Constraining the peptides with a single staple was not sufficient to inhibit RSV infection. However, the insertion of double staples led to the identification of novel short stapled peptides that display nanomolar potency in HEp-2 cells and are exceptionally robust to proteolytic degradation. By replacing each amino acid of the peptides by an alanine, we found that the substitution of residues 506 to 509, located in a patch of polar contacts between HR2 and HR1, severely affected inhibition. Finally, we show that intranasal delivery of the most potent peptide to BALB/c mice significantly decreased RSV infection in upper and lower respiratory tracts. The discovery of this minimal HR2 sequence as a means for inhibition of RSV infection provides the basis for further medicinal chemistry efforts toward developing RSV fusion antivirals.
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spelling pubmed-53656622017-04-12 A Short Double-Stapled Peptide Inhibits Respiratory Syncytial Virus Entry and Spreading Gaillard, Vanessa Galloux, Marie Garcin, Dominique Eléouët, Jean-François Le Goffic, Ronan Larcher, Thibaut Rameix-Welti, Marie-Anne Boukadiri, Abdelhak Héritier, Julien Segura, Jean-Manuel Baechler, Elodie Arrell, Miriam Mottet-Osman, Geneviève Nyanguile, Origène Antimicrob Agents Chemother Antiviral Agents Synthetic peptides derived from the heptad repeat (HR) of fusion (F) proteins can be used as dominant negative inhibitors to inhibit the fusion mechanism of class I viral F proteins. Here, we have performed a stapled-peptide scan across the HR2 domain of the respiratory syncytial virus (RSV) F protein with the aim to identify a minimal domain capable of disrupting the formation of the postfusion six-helix bundle required for viral cell entry. Constraining the peptides with a single staple was not sufficient to inhibit RSV infection. However, the insertion of double staples led to the identification of novel short stapled peptides that display nanomolar potency in HEp-2 cells and are exceptionally robust to proteolytic degradation. By replacing each amino acid of the peptides by an alanine, we found that the substitution of residues 506 to 509, located in a patch of polar contacts between HR2 and HR1, severely affected inhibition. Finally, we show that intranasal delivery of the most potent peptide to BALB/c mice significantly decreased RSV infection in upper and lower respiratory tracts. The discovery of this minimal HR2 sequence as a means for inhibition of RSV infection provides the basis for further medicinal chemistry efforts toward developing RSV fusion antivirals. American Society for Microbiology 2017-03-24 /pmc/articles/PMC5365662/ /pubmed/28137809 http://dx.doi.org/10.1128/AAC.02241-16 Text en Copyright © 2017 Gaillard et al. http://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 (http://creativecommons.org/licenses/by/4.0/) .
spellingShingle Antiviral Agents
Gaillard, Vanessa
Galloux, Marie
Garcin, Dominique
Eléouët, Jean-François
Le Goffic, Ronan
Larcher, Thibaut
Rameix-Welti, Marie-Anne
Boukadiri, Abdelhak
Héritier, Julien
Segura, Jean-Manuel
Baechler, Elodie
Arrell, Miriam
Mottet-Osman, Geneviève
Nyanguile, Origène
A Short Double-Stapled Peptide Inhibits Respiratory Syncytial Virus Entry and Spreading
title A Short Double-Stapled Peptide Inhibits Respiratory Syncytial Virus Entry and Spreading
title_full A Short Double-Stapled Peptide Inhibits Respiratory Syncytial Virus Entry and Spreading
title_fullStr A Short Double-Stapled Peptide Inhibits Respiratory Syncytial Virus Entry and Spreading
title_full_unstemmed A Short Double-Stapled Peptide Inhibits Respiratory Syncytial Virus Entry and Spreading
title_short A Short Double-Stapled Peptide Inhibits Respiratory Syncytial Virus Entry and Spreading
title_sort short double-stapled peptide inhibits respiratory syncytial virus entry and spreading
topic Antiviral Agents
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5365662/
https://www.ncbi.nlm.nih.gov/pubmed/28137809
http://dx.doi.org/10.1128/AAC.02241-16
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