Rationally Designed Interfacial Peptides Are Efficient In Vitro Inhibitors of HIV-1 Capsid Assembly with Antiviral Activity

Virus capsid assembly constitutes an attractive target for the development of antiviral therapies; a few experimental inhibitors of this process for HIV-1 and other viruses have been identified by screening compounds or by selection from chemical libraries. As a different, novel approach we have und...

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Autores principales: Bocanegra, Rebeca, Nevot, María, Doménech, Rosa, López, Inmaculada, Abián, Olga, Rodríguez-Huete, Alicia, Cavasotto, Claudio N., Velázquez-Campoy, Adrián, Gómez, Javier, Martínez, Miguel Ángel, Neira, José Luis, Mateu, Mauricio G.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2011
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3169566/
https://www.ncbi.nlm.nih.gov/pubmed/21931621
http://dx.doi.org/10.1371/journal.pone.0023877
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author Bocanegra, Rebeca
Nevot, María
Doménech, Rosa
López, Inmaculada
Abián, Olga
Rodríguez-Huete, Alicia
Cavasotto, Claudio N.
Velázquez-Campoy, Adrián
Gómez, Javier
Martínez, Miguel Ángel
Neira, José Luis
Mateu, Mauricio G.
author_facet Bocanegra, Rebeca
Nevot, María
Doménech, Rosa
López, Inmaculada
Abián, Olga
Rodríguez-Huete, Alicia
Cavasotto, Claudio N.
Velázquez-Campoy, Adrián
Gómez, Javier
Martínez, Miguel Ángel
Neira, José Luis
Mateu, Mauricio G.
author_sort Bocanegra, Rebeca
collection PubMed
description Virus capsid assembly constitutes an attractive target for the development of antiviral therapies; a few experimental inhibitors of this process for HIV-1 and other viruses have been identified by screening compounds or by selection from chemical libraries. As a different, novel approach we have undertaken the rational design of peptides that could act as competitive assembly inhibitors by mimicking capsid structural elements involved in intersubunit interfaces. Several discrete interfaces involved in formation of the mature HIV-1 capsid through polymerization of the capsid protein CA were targeted. We had previously designed a peptide, CAC1, that represents CA helix 9 (a major part of the dimerization interface) and binds the CA C-terminal domain in solution. Here we have mapped the binding site of CAC1, and shown that it substantially overlaps with the CA dimerization interface. We have also rationally modified CAC1 to increase its solubility and CA-binding affinity, and designed four additional peptides that represent CA helical segments involved in other CA interfaces. We found that peptides CAC1, its derivative CAC1M, and H8 (representing CA helix 8) were able to efficiently inhibit the in vitro assembly of the mature HIV-1 capsid. Cocktails of several peptides, including CAC1 or CAC1M plus H8 or CAI (a previously discovered inhibitor of CA polymerization), or CAC1M+H8+CAI, also abolished capsid assembly, even when every peptide was used at lower, sub-inhibitory doses. To provide a preliminary proof that these designed capsid assembly inhibitors could eventually serve as lead compounds for development of anti-HIV-1 agents, they were transported into cultured cells using a cell-penetrating peptide, and tested for antiviral activity. Peptide cocktails that drastically inhibited capsid assembly in vitro were also able to efficiently inhibit HIV-1 infection ex vivo. This study validates a novel, entirely rational approach for the design of capsid assembly interfacial inhibitors that show antiviral activity.
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spelling pubmed-31695662011-09-19 Rationally Designed Interfacial Peptides Are Efficient In Vitro Inhibitors of HIV-1 Capsid Assembly with Antiviral Activity Bocanegra, Rebeca Nevot, María Doménech, Rosa López, Inmaculada Abián, Olga Rodríguez-Huete, Alicia Cavasotto, Claudio N. Velázquez-Campoy, Adrián Gómez, Javier Martínez, Miguel Ángel Neira, José Luis Mateu, Mauricio G. PLoS One Research Article Virus capsid assembly constitutes an attractive target for the development of antiviral therapies; a few experimental inhibitors of this process for HIV-1 and other viruses have been identified by screening compounds or by selection from chemical libraries. As a different, novel approach we have undertaken the rational design of peptides that could act as competitive assembly inhibitors by mimicking capsid structural elements involved in intersubunit interfaces. Several discrete interfaces involved in formation of the mature HIV-1 capsid through polymerization of the capsid protein CA were targeted. We had previously designed a peptide, CAC1, that represents CA helix 9 (a major part of the dimerization interface) and binds the CA C-terminal domain in solution. Here we have mapped the binding site of CAC1, and shown that it substantially overlaps with the CA dimerization interface. We have also rationally modified CAC1 to increase its solubility and CA-binding affinity, and designed four additional peptides that represent CA helical segments involved in other CA interfaces. We found that peptides CAC1, its derivative CAC1M, and H8 (representing CA helix 8) were able to efficiently inhibit the in vitro assembly of the mature HIV-1 capsid. Cocktails of several peptides, including CAC1 or CAC1M plus H8 or CAI (a previously discovered inhibitor of CA polymerization), or CAC1M+H8+CAI, also abolished capsid assembly, even when every peptide was used at lower, sub-inhibitory doses. To provide a preliminary proof that these designed capsid assembly inhibitors could eventually serve as lead compounds for development of anti-HIV-1 agents, they were transported into cultured cells using a cell-penetrating peptide, and tested for antiviral activity. Peptide cocktails that drastically inhibited capsid assembly in vitro were also able to efficiently inhibit HIV-1 infection ex vivo. This study validates a novel, entirely rational approach for the design of capsid assembly interfacial inhibitors that show antiviral activity. Public Library of Science 2011-09-08 /pmc/articles/PMC3169566/ /pubmed/21931621 http://dx.doi.org/10.1371/journal.pone.0023877 Text en Bocanegra 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, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Bocanegra, Rebeca
Nevot, María
Doménech, Rosa
López, Inmaculada
Abián, Olga
Rodríguez-Huete, Alicia
Cavasotto, Claudio N.
Velázquez-Campoy, Adrián
Gómez, Javier
Martínez, Miguel Ángel
Neira, José Luis
Mateu, Mauricio G.
Rationally Designed Interfacial Peptides Are Efficient In Vitro Inhibitors of HIV-1 Capsid Assembly with Antiviral Activity
title Rationally Designed Interfacial Peptides Are Efficient In Vitro Inhibitors of HIV-1 Capsid Assembly with Antiviral Activity
title_full Rationally Designed Interfacial Peptides Are Efficient In Vitro Inhibitors of HIV-1 Capsid Assembly with Antiviral Activity
title_fullStr Rationally Designed Interfacial Peptides Are Efficient In Vitro Inhibitors of HIV-1 Capsid Assembly with Antiviral Activity
title_full_unstemmed Rationally Designed Interfacial Peptides Are Efficient In Vitro Inhibitors of HIV-1 Capsid Assembly with Antiviral Activity
title_short Rationally Designed Interfacial Peptides Are Efficient In Vitro Inhibitors of HIV-1 Capsid Assembly with Antiviral Activity
title_sort rationally designed interfacial peptides are efficient in vitro inhibitors of hiv-1 capsid assembly with antiviral activity
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3169566/
https://www.ncbi.nlm.nih.gov/pubmed/21931621
http://dx.doi.org/10.1371/journal.pone.0023877
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