Persistence of frequently transmitted drug-resistant HIV-1 variants can be explained by high viral replication capacity

BACKGROUND: In approximately 10% of newly diagnosed individuals in Europe, HIV-1 variants harboring transmitted drug resistance mutations (TDRM) are detected. For some TDRM it has been shown that they revert to wild type while other mutations persist in the absence of therapy. To understand the mech...

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Autores principales: Pingen, Marieke, Wensing, Annemarie MJ, Fransen, Katrien, De Bel, Annelies, de Jong, Dorien, Hoepelman, Andy IM, Magiorkinis, Emmanouil, Paraskevis, Dimitrios, Lunar, Maja M, Poljak, Mario, Nijhuis, Monique, Boucher, Charles AB
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2014
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4263067/
https://www.ncbi.nlm.nih.gov/pubmed/25575025
http://dx.doi.org/10.1186/s12977-014-0105-9
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author Pingen, Marieke
Wensing, Annemarie MJ
Fransen, Katrien
De Bel, Annelies
de Jong, Dorien
Hoepelman, Andy IM
Magiorkinis, Emmanouil
Paraskevis, Dimitrios
Lunar, Maja M
Poljak, Mario
Nijhuis, Monique
Boucher, Charles AB
author_facet Pingen, Marieke
Wensing, Annemarie MJ
Fransen, Katrien
De Bel, Annelies
de Jong, Dorien
Hoepelman, Andy IM
Magiorkinis, Emmanouil
Paraskevis, Dimitrios
Lunar, Maja M
Poljak, Mario
Nijhuis, Monique
Boucher, Charles AB
author_sort Pingen, Marieke
collection PubMed
description BACKGROUND: In approximately 10% of newly diagnosed individuals in Europe, HIV-1 variants harboring transmitted drug resistance mutations (TDRM) are detected. For some TDRM it has been shown that they revert to wild type while other mutations persist in the absence of therapy. To understand the mechanisms explaining persistence we investigated the in vivo evolution of frequently transmitted HIV-1 variants and their impact on in vitro replicative capacity. RESULTS: We selected 31 individuals infected with HIV-1 harboring frequently observed TDRM such as M41L or K103N in reverse transcriptase (RT) or M46L in protease. In all these samples, polymorphisms at non-TDRM positions were present at baseline (median protease: 5, RT: 6). Extensive analysis of viral evolution of protease and RT demonstrated that the majority of TDRM (51/55) persisted for at least a year and even up to eight years in the plasma. During follow-up only limited selection of additional polymorphisms was observed (median: 1). To investigate the impact of frequently observed TDRM on the replication capacity, mutant viruses were constructed with the most frequently encountered TDRM as site-directed mutants in the genetic background of the lab strain HXB2. In addition, viruses containing patient-derived protease or RT harboring similar TDRM were made. The replicative capacity of all viral variants was determined by infecting peripheral blood mononuclear cells and subsequently monitoring virus replication. The majority of site-directed mutations (M46I/M46L in protease and M41L, M41L + T215Y and K103N in RT) decreased viral replicative capacity; only protease mutation L90M did not hamper viral replication. Interestingly, most patient-derived viruses had a higher in vitro replicative capacity than the corresponding site-directed mutant viruses. CONCLUSIONS: We demonstrate limited in vivo evolution of protease and RT harbouring frequently observed TDRM in the plasma. This is in line with the high in vitro replication capacity of patient-derived viruses harbouring TDRM compared to site-directed mutant viruses harbouring TDRM. As site-directed mutant viruses have a lower replication capacity than the patient-derived viruses with similar mutational patterns, we propose that (baseline) polymorphisms function as compensatory mutations improving viral replication capacity.
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spelling pubmed-42630672014-12-12 Persistence of frequently transmitted drug-resistant HIV-1 variants can be explained by high viral replication capacity Pingen, Marieke Wensing, Annemarie MJ Fransen, Katrien De Bel, Annelies de Jong, Dorien Hoepelman, Andy IM Magiorkinis, Emmanouil Paraskevis, Dimitrios Lunar, Maja M Poljak, Mario Nijhuis, Monique Boucher, Charles AB Retrovirology Research BACKGROUND: In approximately 10% of newly diagnosed individuals in Europe, HIV-1 variants harboring transmitted drug resistance mutations (TDRM) are detected. For some TDRM it has been shown that they revert to wild type while other mutations persist in the absence of therapy. To understand the mechanisms explaining persistence we investigated the in vivo evolution of frequently transmitted HIV-1 variants and their impact on in vitro replicative capacity. RESULTS: We selected 31 individuals infected with HIV-1 harboring frequently observed TDRM such as M41L or K103N in reverse transcriptase (RT) or M46L in protease. In all these samples, polymorphisms at non-TDRM positions were present at baseline (median protease: 5, RT: 6). Extensive analysis of viral evolution of protease and RT demonstrated that the majority of TDRM (51/55) persisted for at least a year and even up to eight years in the plasma. During follow-up only limited selection of additional polymorphisms was observed (median: 1). To investigate the impact of frequently observed TDRM on the replication capacity, mutant viruses were constructed with the most frequently encountered TDRM as site-directed mutants in the genetic background of the lab strain HXB2. In addition, viruses containing patient-derived protease or RT harboring similar TDRM were made. The replicative capacity of all viral variants was determined by infecting peripheral blood mononuclear cells and subsequently monitoring virus replication. The majority of site-directed mutations (M46I/M46L in protease and M41L, M41L + T215Y and K103N in RT) decreased viral replicative capacity; only protease mutation L90M did not hamper viral replication. Interestingly, most patient-derived viruses had a higher in vitro replicative capacity than the corresponding site-directed mutant viruses. CONCLUSIONS: We demonstrate limited in vivo evolution of protease and RT harbouring frequently observed TDRM in the plasma. This is in line with the high in vitro replication capacity of patient-derived viruses harbouring TDRM compared to site-directed mutant viruses harbouring TDRM. As site-directed mutant viruses have a lower replication capacity than the patient-derived viruses with similar mutational patterns, we propose that (baseline) polymorphisms function as compensatory mutations improving viral replication capacity. BioMed Central 2014-11-29 /pmc/articles/PMC4263067/ /pubmed/25575025 http://dx.doi.org/10.1186/s12977-014-0105-9 Text en © Pingen et al.; licensee BioMed Central Ltd. 2014 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 work is properly credited. The Creative Commons Public Domain Dedication waiver (http://creativecommons.org/publicdomain/zero/1.0/) applies to the data made available in this article, unless otherwise stated.
spellingShingle Research
Pingen, Marieke
Wensing, Annemarie MJ
Fransen, Katrien
De Bel, Annelies
de Jong, Dorien
Hoepelman, Andy IM
Magiorkinis, Emmanouil
Paraskevis, Dimitrios
Lunar, Maja M
Poljak, Mario
Nijhuis, Monique
Boucher, Charles AB
Persistence of frequently transmitted drug-resistant HIV-1 variants can be explained by high viral replication capacity
title Persistence of frequently transmitted drug-resistant HIV-1 variants can be explained by high viral replication capacity
title_full Persistence of frequently transmitted drug-resistant HIV-1 variants can be explained by high viral replication capacity
title_fullStr Persistence of frequently transmitted drug-resistant HIV-1 variants can be explained by high viral replication capacity
title_full_unstemmed Persistence of frequently transmitted drug-resistant HIV-1 variants can be explained by high viral replication capacity
title_short Persistence of frequently transmitted drug-resistant HIV-1 variants can be explained by high viral replication capacity
title_sort persistence of frequently transmitted drug-resistant hiv-1 variants can be explained by high viral replication capacity
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4263067/
https://www.ncbi.nlm.nih.gov/pubmed/25575025
http://dx.doi.org/10.1186/s12977-014-0105-9
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