High prevalence of integrase mutation L74I in West African HIV-1 subtypes prior to integrase inhibitor treatment

OBJECTIVES: HIV-1 integrase inhibitors are recommended as first-line therapy by WHO, though efficacy and resistance data for non-B subtypes are limited. Two recent trials have identified the integrase L74I mutation to be associated with integrase inhibitor treatment failure in HIV-1 non-B subtypes....

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Autores principales: El Bouzidi, Kate, Kemp, Steven A, Datir, Rawlings P, Murtala-Ibrahim, Fati, Aliyu, Ahmad, Kwaghe, Vivian, Frampton, Dan, Roy, Sunando, Breuer, Judith, Sabin, Caroline A, Ogbanufe, Obinna, Charurat, Man E, Bonsall, David, Golubchik, Tanya, Fraser, Christophe, Dakum, Patrick, Ndembi, Nicaise, Gupta, Ravindra K
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Oxford University Press 2020
Materias:
Original Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7225870/
https://www.ncbi.nlm.nih.gov/pubmed/32105319
http://dx.doi.org/10.1093/jac/dkaa033
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author El Bouzidi, Kate
Kemp, Steven A
Datir, Rawlings P
Murtala-Ibrahim, Fati
Aliyu, Ahmad
Kwaghe, Vivian
Frampton, Dan
Roy, Sunando
Breuer, Judith
Sabin, Caroline A
Ogbanufe, Obinna
Charurat, Man E
Bonsall, David
Golubchik, Tanya
Fraser, Christophe
Dakum, Patrick
Ndembi, Nicaise
Gupta, Ravindra K
author_facet El Bouzidi, Kate
Kemp, Steven A
Datir, Rawlings P
Murtala-Ibrahim, Fati
Aliyu, Ahmad
Kwaghe, Vivian
Frampton, Dan
Roy, Sunando
Breuer, Judith
Sabin, Caroline A
Ogbanufe, Obinna
Charurat, Man E
Bonsall, David
Golubchik, Tanya
Fraser, Christophe
Dakum, Patrick
Ndembi, Nicaise
Gupta, Ravindra K
author_sort El Bouzidi, Kate
collection PubMed
description OBJECTIVES: HIV-1 integrase inhibitors are recommended as first-line therapy by WHO, though efficacy and resistance data for non-B subtypes are limited. Two recent trials have identified the integrase L74I mutation to be associated with integrase inhibitor treatment failure in HIV-1 non-B subtypes. We sought to define the prevalence of integrase resistance mutations, including L74I, in West Africa. METHODS: We studied a Nigerian cohort of recipients prior to and during receipt of second-line PI-based therapy, who were integrase inhibitor-naive. Illumina next-generation sequencing with target enrichment was used on stored plasma samples. Drug resistance was interpreted using the Stanford Resistance Database and the IAS-USA 2019 mutation lists. RESULTS: Of 115 individuals, 59.1% harboured CRF02_AG HIV-1 and 40.9% harboured subtype G HIV-1. Four participants had major IAS-USA integrase resistance-associated mutations detected at low levels (2%–5% frequency). Two had Q148K minority variants and two had R263K (one of whom also had L74I). L74I was detected in plasma samples at over 2% frequency in 40% (46/115). Twelve (26.1%) had low-level minority variants of between 2% and 20% of the viral population sampled. The remaining 34 (73.9%) had L74I present at >20% frequency. L74I was more common among those with subtype G infection (55.3%, 26/47) than those with CRF02_AG infection (29.4%, 20/68) (P = 0.005). CONCLUSIONS: HIV-1 subtypes circulating in West Africa appear to have very low prevalence of major integrase mutations, but significant prevalence of L74I. A combination of in vitro and clinical studies is warranted to understand the potential implications.
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spelling pubmed-72258702020-05-19 High prevalence of integrase mutation L74I in West African HIV-1 subtypes prior to integrase inhibitor treatment El Bouzidi, Kate Kemp, Steven A Datir, Rawlings P Murtala-Ibrahim, Fati Aliyu, Ahmad Kwaghe, Vivian Frampton, Dan Roy, Sunando Breuer, Judith Sabin, Caroline A Ogbanufe, Obinna Charurat, Man E Bonsall, David Golubchik, Tanya Fraser, Christophe Dakum, Patrick Ndembi, Nicaise Gupta, Ravindra K J Antimicrob Chemother Original Research OBJECTIVES: HIV-1 integrase inhibitors are recommended as first-line therapy by WHO, though efficacy and resistance data for non-B subtypes are limited. Two recent trials have identified the integrase L74I mutation to be associated with integrase inhibitor treatment failure in HIV-1 non-B subtypes. We sought to define the prevalence of integrase resistance mutations, including L74I, in West Africa. METHODS: We studied a Nigerian cohort of recipients prior to and during receipt of second-line PI-based therapy, who were integrase inhibitor-naive. Illumina next-generation sequencing with target enrichment was used on stored plasma samples. Drug resistance was interpreted using the Stanford Resistance Database and the IAS-USA 2019 mutation lists. RESULTS: Of 115 individuals, 59.1% harboured CRF02_AG HIV-1 and 40.9% harboured subtype G HIV-1. Four participants had major IAS-USA integrase resistance-associated mutations detected at low levels (2%–5% frequency). Two had Q148K minority variants and two had R263K (one of whom also had L74I). L74I was detected in plasma samples at over 2% frequency in 40% (46/115). Twelve (26.1%) had low-level minority variants of between 2% and 20% of the viral population sampled. The remaining 34 (73.9%) had L74I present at >20% frequency. L74I was more common among those with subtype G infection (55.3%, 26/47) than those with CRF02_AG infection (29.4%, 20/68) (P = 0.005). CONCLUSIONS: HIV-1 subtypes circulating in West Africa appear to have very low prevalence of major integrase mutations, but significant prevalence of L74I. A combination of in vitro and clinical studies is warranted to understand the potential implications. Oxford University Press 2020-06 2020-02-27 /pmc/articles/PMC7225870/ /pubmed/32105319 http://dx.doi.org/10.1093/jac/dkaa033 Text en © The Author(s) 2020. Published by Oxford University Press on behalf of the British Society for Antimicrobial Chemotherapy. http://creativecommons.org/licenses/by/4.0/ 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 reuse, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Original Research
El Bouzidi, Kate
Kemp, Steven A
Datir, Rawlings P
Murtala-Ibrahim, Fati
Aliyu, Ahmad
Kwaghe, Vivian
Frampton, Dan
Roy, Sunando
Breuer, Judith
Sabin, Caroline A
Ogbanufe, Obinna
Charurat, Man E
Bonsall, David
Golubchik, Tanya
Fraser, Christophe
Dakum, Patrick
Ndembi, Nicaise
Gupta, Ravindra K
High prevalence of integrase mutation L74I in West African HIV-1 subtypes prior to integrase inhibitor treatment
title High prevalence of integrase mutation L74I in West African HIV-1 subtypes prior to integrase inhibitor treatment
title_full High prevalence of integrase mutation L74I in West African HIV-1 subtypes prior to integrase inhibitor treatment
title_fullStr High prevalence of integrase mutation L74I in West African HIV-1 subtypes prior to integrase inhibitor treatment
title_full_unstemmed High prevalence of integrase mutation L74I in West African HIV-1 subtypes prior to integrase inhibitor treatment
title_short High prevalence of integrase mutation L74I in West African HIV-1 subtypes prior to integrase inhibitor treatment
title_sort high prevalence of integrase mutation l74i in west african hiv-1 subtypes prior to integrase inhibitor treatment
topic Original Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7225870/
https://www.ncbi.nlm.nih.gov/pubmed/32105319
http://dx.doi.org/10.1093/jac/dkaa033
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