G140S/Q148R and N155H mutations render HIV-2 Integrase resistant to Raltegravir whereas Y143C does not

BACKGROUND: HIV-2 is endemic in West Africa and has spread throughout Europe. However, the alternatives for HIV-2-infected patients are more limited than for HIV-1. Raltegravir, an integrase inhibitor, is active against wild-type HIV-2, with a susceptibility to this drug similar to that of HIV-1, an...

Descripción completa

Detalles Bibliográficos
Autores principales: Ni, Xiao-Ju, Delelis, Olivier, Charpentier, Charlotte, Storto, Alexandre, Collin, Gilles, Damond, Florence, Descamps, Diane, Mouscadet, Jean-François
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2011
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3170264/
https://www.ncbi.nlm.nih.gov/pubmed/21854605
http://dx.doi.org/10.1186/1742-4690-8-68
_version_ 1782211598914420736
author Ni, Xiao-Ju
Delelis, Olivier
Charpentier, Charlotte
Storto, Alexandre
Collin, Gilles
Damond, Florence
Descamps, Diane
Mouscadet, Jean-François
author_facet Ni, Xiao-Ju
Delelis, Olivier
Charpentier, Charlotte
Storto, Alexandre
Collin, Gilles
Damond, Florence
Descamps, Diane
Mouscadet, Jean-François
author_sort Ni, Xiao-Ju
collection PubMed
description BACKGROUND: HIV-2 is endemic in West Africa and has spread throughout Europe. However, the alternatives for HIV-2-infected patients are more limited than for HIV-1. Raltegravir, an integrase inhibitor, is active against wild-type HIV-2, with a susceptibility to this drug similar to that of HIV-1, and is therefore a promising option for use in the treatment of HIV-2-infected patients. Recent studies have shown that HIV-2 resistance to raltegravir involves one of three resistance mutations, N155H, Q148R/H and Y143C, previously identified as resistance determinants in the HIV-1 integrase coding sequence. The resistance of HIV-1 IN has been confirmed in vitro for mutated enzymes harboring these mutations, but no such confirmation has yet been obtained for HIV-2. RESULTS: The integrase coding sequence was amplified from plasma samples collected from ten patients infected with HIV-2 viruses, of whom three RAL-naïve and seven on RAL-based treatment at the time of virological failure. The genomes of the resistant strains were cloned and three patterns involving N155H, G140S/Q148R or Y143C mutations were identified. Study of the susceptibility of integrases, either amplified from clinical isolates or obtained by mutagenesis demonstrated that mutations at positions 155 and 148 render the integrase resistant to RAL. The G140S mutation conferred little resistance, but compensated for the catalytic defect due to the Q148R mutation. Conversely, Y143C alone did not confer resistance to RAL unless E92Q is also present. Furthermore, the introduction of the Y143C mutation into the N155H resistant background decreased the resistance level of enzymes containing the N155H mutation. CONCLUSION: This study confirms that HIV-2 resistance to RAL is due to the N155H, G140S/Q148R or E92Q/Y143C mutations. The N155H and G140S/Q148R mutations make similar contributions to resistance in both HIV-1 and HIV-2, but Y143C is not sufficient to account for the resistance of HIV-2 genomes harboring this mutation. For Y143C to confer resistance in vitro, it must be accompanied by E92Q, which therefore plays a more important role in the HIV-2 context than in the HIV-1 context. Finally, the Y143C mutation counteracts the resistance conferred by the N155H mutation, probably accounting for the lack of detection of these mutations together in a single genome.
format Online
Article
Text
id pubmed-3170264
institution National Center for Biotechnology Information
language English
publishDate 2011
publisher BioMed Central
record_format MEDLINE/PubMed
spelling pubmed-31702642011-09-10 G140S/Q148R and N155H mutations render HIV-2 Integrase resistant to Raltegravir whereas Y143C does not Ni, Xiao-Ju Delelis, Olivier Charpentier, Charlotte Storto, Alexandre Collin, Gilles Damond, Florence Descamps, Diane Mouscadet, Jean-François Retrovirology Research BACKGROUND: HIV-2 is endemic in West Africa and has spread throughout Europe. However, the alternatives for HIV-2-infected patients are more limited than for HIV-1. Raltegravir, an integrase inhibitor, is active against wild-type HIV-2, with a susceptibility to this drug similar to that of HIV-1, and is therefore a promising option for use in the treatment of HIV-2-infected patients. Recent studies have shown that HIV-2 resistance to raltegravir involves one of three resistance mutations, N155H, Q148R/H and Y143C, previously identified as resistance determinants in the HIV-1 integrase coding sequence. The resistance of HIV-1 IN has been confirmed in vitro for mutated enzymes harboring these mutations, but no such confirmation has yet been obtained for HIV-2. RESULTS: The integrase coding sequence was amplified from plasma samples collected from ten patients infected with HIV-2 viruses, of whom three RAL-naïve and seven on RAL-based treatment at the time of virological failure. The genomes of the resistant strains were cloned and three patterns involving N155H, G140S/Q148R or Y143C mutations were identified. Study of the susceptibility of integrases, either amplified from clinical isolates or obtained by mutagenesis demonstrated that mutations at positions 155 and 148 render the integrase resistant to RAL. The G140S mutation conferred little resistance, but compensated for the catalytic defect due to the Q148R mutation. Conversely, Y143C alone did not confer resistance to RAL unless E92Q is also present. Furthermore, the introduction of the Y143C mutation into the N155H resistant background decreased the resistance level of enzymes containing the N155H mutation. CONCLUSION: This study confirms that HIV-2 resistance to RAL is due to the N155H, G140S/Q148R or E92Q/Y143C mutations. The N155H and G140S/Q148R mutations make similar contributions to resistance in both HIV-1 and HIV-2, but Y143C is not sufficient to account for the resistance of HIV-2 genomes harboring this mutation. For Y143C to confer resistance in vitro, it must be accompanied by E92Q, which therefore plays a more important role in the HIV-2 context than in the HIV-1 context. Finally, the Y143C mutation counteracts the resistance conferred by the N155H mutation, probably accounting for the lack of detection of these mutations together in a single genome. BioMed Central 2011-08-19 /pmc/articles/PMC3170264/ /pubmed/21854605 http://dx.doi.org/10.1186/1742-4690-8-68 Text en Copyright ©2011 Ni et al; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/2.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research
Ni, Xiao-Ju
Delelis, Olivier
Charpentier, Charlotte
Storto, Alexandre
Collin, Gilles
Damond, Florence
Descamps, Diane
Mouscadet, Jean-François
G140S/Q148R and N155H mutations render HIV-2 Integrase resistant to Raltegravir whereas Y143C does not
title G140S/Q148R and N155H mutations render HIV-2 Integrase resistant to Raltegravir whereas Y143C does not
title_full G140S/Q148R and N155H mutations render HIV-2 Integrase resistant to Raltegravir whereas Y143C does not
title_fullStr G140S/Q148R and N155H mutations render HIV-2 Integrase resistant to Raltegravir whereas Y143C does not
title_full_unstemmed G140S/Q148R and N155H mutations render HIV-2 Integrase resistant to Raltegravir whereas Y143C does not
title_short G140S/Q148R and N155H mutations render HIV-2 Integrase resistant to Raltegravir whereas Y143C does not
title_sort g140s/q148r and n155h mutations render hiv-2 integrase resistant to raltegravir whereas y143c does not
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3170264/
https://www.ncbi.nlm.nih.gov/pubmed/21854605
http://dx.doi.org/10.1186/1742-4690-8-68
work_keys_str_mv AT nixiaoju g140sq148randn155hmutationsrenderhiv2integraseresistanttoraltegravirwhereasy143cdoesnot
AT delelisolivier g140sq148randn155hmutationsrenderhiv2integraseresistanttoraltegravirwhereasy143cdoesnot
AT charpentiercharlotte g140sq148randn155hmutationsrenderhiv2integraseresistanttoraltegravirwhereasy143cdoesnot
AT stortoalexandre g140sq148randn155hmutationsrenderhiv2integraseresistanttoraltegravirwhereasy143cdoesnot
AT collingilles g140sq148randn155hmutationsrenderhiv2integraseresistanttoraltegravirwhereasy143cdoesnot
AT damondflorence g140sq148randn155hmutationsrenderhiv2integraseresistanttoraltegravirwhereasy143cdoesnot
AT descampsdiane g140sq148randn155hmutationsrenderhiv2integraseresistanttoraltegravirwhereasy143cdoesnot
AT mouscadetjeanfrancois g140sq148randn155hmutationsrenderhiv2integraseresistanttoraltegravirwhereasy143cdoesnot

Ejemplares similares