Integrase resistance emergence with dolutegravir/lamivudine with prior HIV-1 suppression
Integrase resistance has not been reported with co-formulated dolutegravir/lamivudine in clinical trials or real-life cohorts. We aim to report, to the best of our knowledge, the first case of selection of the key integrase mutation R263K in a subject treated with this regimen started as a switch st...
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| Published in | Journal of antimicrobial chemotherapy Vol. 77; no. 6; pp. 1738 - 1740 |
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| Main Authors | , , , , , , , |
| Format | Journal Article |
| Language | English |
| Published |
England
29.05.2022
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| Subjects | |
| Online Access | Get full text |
| ISSN | 0305-7453 1460-2091 1460-2091 |
| DOI | 10.1093/jac/dkac082 |
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| Abstract | Integrase resistance has not been reported with co-formulated dolutegravir/lamivudine in clinical trials or real-life cohorts. We aim to report, to the best of our knowledge, the first case of selection of the key integrase mutation R263K in a subject treated with this regimen started as a switch strategy with undetectable plasma HIV-1 viraemia.
Clinical case report.
A patient with long-term suppressed HIV-1 viraemia (<50 copies/mL) with no known risk factors for virological failure and never exposed previously to an integrase inhibitor developed virological failure (consecutive plasma HIV-1 RNA 149 and 272 copies/mL) with 322 CD4 cells/mm3 despite good treatment adherence. He was receiving the anticonvulsant clobazam, considered to have a potential weak interaction with dolutegravir, unlikely to require a dose adjustment. Plasma HIV-1 genotypic deep sequencing (Vela System) revealed the emergence of R263K (79.6%) and S230N (99.4%) mutations in the integrase region (intermediate resistance to dolutegravir, score = 30 Stanford HIVDB 9.0). The reverse transcriptase and protease regions could not be amplified due to low viral loads. PBMC DNA deep sequencing performed some months later revealed mutations M184I (14.29%) and M230I (6.25%) in the reverse transcriptase and G163R (9.77%) and S230N (98.8%) in the integrase. R263K was only found at extremely low levels (0.07%).
This case illustrates that integrase resistance can emerge in patients treated with co-formulated dolutegravir/lamivudine and raises awareness of the need to carefully consider and monitor drug-drug interactions, even when regarded as having a low potential, in subjects treated with dolutegravir/lamivudine. |
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| AbstractList | Integrase resistance has not been reported with co-formulated dolutegravir/lamivudine in clinical trials or real-life cohorts. We aim to report, to the best of our knowledge, the first case of selection of the key integrase mutation R263K in a subject treated with this regimen started as a switch strategy with undetectable plasma HIV-1 viraemia.
Clinical case report.
A patient with long-term suppressed HIV-1 viraemia (<50 copies/mL) with no known risk factors for virological failure and never exposed previously to an integrase inhibitor developed virological failure (consecutive plasma HIV-1 RNA 149 and 272 copies/mL) with 322 CD4 cells/mm3 despite good treatment adherence. He was receiving the anticonvulsant clobazam, considered to have a potential weak interaction with dolutegravir, unlikely to require a dose adjustment. Plasma HIV-1 genotypic deep sequencing (Vela System) revealed the emergence of R263K (79.6%) and S230N (99.4%) mutations in the integrase region (intermediate resistance to dolutegravir, score = 30 Stanford HIVDB 9.0). The reverse transcriptase and protease regions could not be amplified due to low viral loads. PBMC DNA deep sequencing performed some months later revealed mutations M184I (14.29%) and M230I (6.25%) in the reverse transcriptase and G163R (9.77%) and S230N (98.8%) in the integrase. R263K was only found at extremely low levels (0.07%).
This case illustrates that integrase resistance can emerge in patients treated with co-formulated dolutegravir/lamivudine and raises awareness of the need to carefully consider and monitor drug-drug interactions, even when regarded as having a low potential, in subjects treated with dolutegravir/lamivudine. Integrase resistance has not been reported with co-formulated dolutegravir/lamivudine in clinical trials or real-life cohorts. We aim to report, to the best of our knowledge, the first case of selection of the key integrase mutation R263K in a subject treated with this regimen started as a switch strategy with undetectable plasma HIV-1 viraemia.OBJECTIVESIntegrase resistance has not been reported with co-formulated dolutegravir/lamivudine in clinical trials or real-life cohorts. We aim to report, to the best of our knowledge, the first case of selection of the key integrase mutation R263K in a subject treated with this regimen started as a switch strategy with undetectable plasma HIV-1 viraemia.Clinical case report.METHODSClinical case report.A patient with long-term suppressed HIV-1 viraemia (<50 copies/mL) with no known risk factors for virological failure and never exposed previously to an integrase inhibitor developed virological failure (consecutive plasma HIV-1 RNA 149 and 272 copies/mL) with 322 CD4 cells/mm3 despite good treatment adherence. He was receiving the anticonvulsant clobazam, considered to have a potential weak interaction with dolutegravir, unlikely to require a dose adjustment. Plasma HIV-1 genotypic deep sequencing (Vela System) revealed the emergence of R263K (79.6%) and S230N (99.4%) mutations in the integrase region (intermediate resistance to dolutegravir, score = 30 Stanford HIVDB 9.0). The reverse transcriptase and protease regions could not be amplified due to low viral loads. PBMC DNA deep sequencing performed some months later revealed mutations M184I (14.29%) and M230I (6.25%) in the reverse transcriptase and G163R (9.77%) and S230N (98.8%) in the integrase. R263K was only found at extremely low levels (0.07%).RESULTSA patient with long-term suppressed HIV-1 viraemia (<50 copies/mL) with no known risk factors for virological failure and never exposed previously to an integrase inhibitor developed virological failure (consecutive plasma HIV-1 RNA 149 and 272 copies/mL) with 322 CD4 cells/mm3 despite good treatment adherence. He was receiving the anticonvulsant clobazam, considered to have a potential weak interaction with dolutegravir, unlikely to require a dose adjustment. Plasma HIV-1 genotypic deep sequencing (Vela System) revealed the emergence of R263K (79.6%) and S230N (99.4%) mutations in the integrase region (intermediate resistance to dolutegravir, score = 30 Stanford HIVDB 9.0). The reverse transcriptase and protease regions could not be amplified due to low viral loads. PBMC DNA deep sequencing performed some months later revealed mutations M184I (14.29%) and M230I (6.25%) in the reverse transcriptase and G163R (9.77%) and S230N (98.8%) in the integrase. R263K was only found at extremely low levels (0.07%).This case illustrates that integrase resistance can emerge in patients treated with co-formulated dolutegravir/lamivudine and raises awareness of the need to carefully consider and monitor drug-drug interactions, even when regarded as having a low potential, in subjects treated with dolutegravir/lamivudine.CONCLUSIONSThis case illustrates that integrase resistance can emerge in patients treated with co-formulated dolutegravir/lamivudine and raises awareness of the need to carefully consider and monitor drug-drug interactions, even when regarded as having a low potential, in subjects treated with dolutegravir/lamivudine. |
| Author | Revollo, Boris Noguera-Julián, Marc Paredes, Roger de la Mora, Lorena García, Federico Llibre, Josep M. Parera, Mariona Viñuela, Laura |
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| References_xml | – volume: 66 start-page: 1689 year: 2018 ident: 2022053122483062800_dkac082-B6 article-title: ACTG A5353: a pilot study of dolutegravir plus lamivudine for initial treatment of human immunodeficiency virus-1 (HIV-1)-infected participants with HIV-1 RNA <500000 copies/mL publication-title: Clin Infect Dis doi: 10.1093/cid/cix1083 – volume: 71 start-page: 1920 year: 2020 ident: 2022053122483062800_dkac082-B1 article-title: Efficacy and safety of switching to dolutegravir/lamivudine fixed-dose 2-drug regimen vs continuing a tenofovir alafenamide-based 3-or 4-drug regimen for maintenance of virologic suppression in adults living with human immunodeficiency virus type 1: phase 3, randomized, noninferiority TANGO study publication-title: Clin Infect Dis doi: 10.1093/cid/ciz1243 – volume-title: IAS Conference on HIV Science, 2021 ident: 2022053122483062800_dkac082-B2 article-title: Switching to the 2-drug regimen of dolutegravir/lamivudine (DTG/3TC) fixed-dose combination is non-inferior to continuing a 3-drug regimen through 48 weeks in a randomized clinical trial (SALSA) – volume: 225 start-page: 502 year: 2022 ident: 2022053122483062800_dkac082-B10 article-title: Kinetics of archived M184V mutation in treatment-experienced virally suppressed HIV-infected patients publication-title: J Infect Dis doi: 10.1093/infdis/jiab413 – volume: 22 start-page: 191 year: 2016 ident: 2022053122483062800_dkac082-B12 article-title: Contribution of APOBEC3G/F activity to the development of low-abundance drug-resistant human immunodeficiency virus type 1 variants publication-title: Clin Microbiol Infect doi: 10.1016/j.cmi.2015.10.004 – volume: 36 start-page: 39 year: 2022 ident: 2022053122483062800_dkac082-B7 article-title: Three-year durable efficacy of dolutegravir plus lamivudine in antiretroviral therapy-naive adults with HIV-1 infection publication-title: AIDS doi: 10.1097/QAD.0000000000003070 – volume: 73 start-page: 2141 year: 2018 ident: 2022053122483062800_dkac082-B11 article-title: Dynamics of drug resistance-associated mutations in HIV-1 DNA reverse transcriptase sequence during effective ART publication-title: J Antimicrob Chemother doi: 10.1093/jac/dky130 – volume: 16 start-page: 18472 year: 2013 ident: 2022053122483062800_dkac082-B14 article-title: Human APOBEC3G-mediated hypermutation is associated with antiretroviral therapy failure in HIV-1 subtype C-infected individuals publication-title: J Int AIDS Soc doi: 10.7448/IAS.16.1.18472 – volume-title: Conference on Retroviruses and Opportunistic Infections, 2021 ident: 2022053122483062800_dkac082-B9 article-title: The impact of M184V on the virological efficacy of switch to 3TC/DTG in real life – volume: 32 start-page: 340 year: 2012 ident: 2022053122483062800_dkac082-B3 article-title: Pharmacokinetic drug interactions between clobazam and drugs metabolized by cytochrome P450 isoenzymes publication-title: Pharmacotherapy doi: 10.1002/j.1875-9114.2012.01028.x – ident: 2022053122483062800_dkac082-B5 article-title: Switching to DTG/3TC fixed-dose combination (FDC) is non-inferior to continuing a TAF-based regimen in maintaining virologic suppression through 144 weeks (TANGO study). IDWeek, 2021. #900 – ident: 2022053122483062800_dkac082-B8 article-title: Dovato EPAR Product Information. Last Update 27 November 2021. Accessed 17 December 2021 – volume: 72 start-page: 2831 year: 2017 ident: 2022053122483062800_dkac082-B13 article-title: HIV-1 DNA ultra-deep sequencing analysis at initiation of the dual therapy dolutegravir + lamivudine in the maintenance DOLULAM pilot study publication-title: J Antimicrob Chemother doi: 10.1093/jac/dkx233 – ident: 2022053122483062800_dkac082-B4 article-title: Accessed 17 December 2021 |
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| SubjectTerms | Drug Resistance, Viral - genetics Heterocyclic Compounds, 3-Ring - adverse effects HIV Infections - drug therapy HIV Integrase Inhibitors - pharmacology HIV Integrase Inhibitors - therapeutic use HIV Seropositivity - drug therapy HIV-1 - genetics Humans Integrases Lamivudine - therapeutic use Leukocytes, Mononuclear Male Oxazines - therapeutic use Piperazines Pyridones - therapeutic use RNA-Directed DNA Polymerase Viremia - drug therapy |
| Title | Integrase resistance emergence with dolutegravir/lamivudine with prior HIV-1 suppression |
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