Third-line antiretroviral therapy, including raltegravir (RAL), darunavir (DRV/r) and/or etravirine (ETR), is well tolerated and achieves durable virologic suppression over 144 weeks in resource-limited settings: ACTG A5288 strategy trial

Anchalee Avihingsanon; Michael D Hughes; Robert Salata; Catherine Godfrey; Caitlyn McCarthy; Peter Mugyenyi; Evelyn Hogg; Robert Gross; Sandra W Cardoso; Aggrey Bukuru; Mumbi Makanga; Sharlaa Badal-Aesen; Vidya Mave; Beatrice Wangari Ndege; Sandy Nerette Fontain; Wadzanai Samaneka; Rode Secours; Marije Van Schalkwyk; Rosie Mngqibisa; Lerato Mohapi; Javier Valencia; Patcharaphan Sugandhavesa; Esmelda Montalban; Cornelius Munyanga; Maganizo Chagomerana; Breno R Santos; Nagalingeswaran Kumarasamy; Cecilia Kanyama; Robert T Schooley; John W Mellors; Carole L Wallis; Ann C Collier; Beatriz Grinsztejn; A5288 Study team

doi:10.1002/jia2.25905

Third-line antiretroviral therapy, including raltegravir (RAL), darunavir (DRV/r) and/or etravirine (ETR), is well tolerated and achieves durable virologic suppression over 144 weeks in resource-limited settings: ACTG A5288 strategy trial

J Int AIDS Soc. 2022 Jun;25(6):e25905. doi: 10.1002/jia2.25905.

Authors

Anchalee Avihingsanon¹, Michael D Hughes², Robert Salata³, Catherine Godfrey⁴, Caitlyn McCarthy², Peter Mugyenyi⁵, Evelyn Hogg⁶, Robert Gross⁷, Sandra W Cardoso⁸, Aggrey Bukuru⁵, Mumbi Makanga⁹, Sharlaa Badal-Aesen¹⁰, Vidya Mave¹¹, Beatrice Wangari Ndege¹², Sandy Nerette Fontain¹³, Wadzanai Samaneka¹⁴, Rode Secours¹³, Marije Van Schalkwyk¹⁵, Rosie Mngqibisa¹⁶, Lerato Mohapi¹⁷, Javier Valencia¹⁸, Patcharaphan Sugandhavesa¹⁹, Esmelda Montalban²⁰, Cornelius Munyanga²¹, Maganizo Chagomerana²¹, Breno R Santos²², Nagalingeswaran Kumarasamy²³, Cecilia Kanyama²¹, Robert T Schooley²⁴, John W Mellors²⁵, Carole L Wallis²⁶, Ann C Collier²⁷, Beatriz Grinsztejn⁸; A5288 Study team

Affiliations

¹ HIV-NAT, Thai Red Cross AIDS Research Centre and Centre of Excellence in Tuberculosis, Faculty of Medicine, Chulalongkorn University, Bangkok, Thailand.
² Center for Biostatistics in AIDS Research in the Department of Biostatistics, Harvard T H Chan School of Public Health, Boston, Massachusetts, USA.
³ Case Western Reserve University, Cleveland, Ohio, USA.
⁴ Division of AIDS, National Institutes of Allergy and Infectious Disease, National Institutes of Health, Bethesda, Maryland, USA.
⁵ Joint Clinical Research Center, Kampala, Uganda.
⁶ Social & Scientific Systems, Inc., a DLH Holdings Company, Silver Spring, Maryland, USA.
⁷ Center for Clinical Epidemiology and Biostatistics, University of Pennsylvania, Philadelphia, Pennsylvania, USA.
⁸ Instituto Nacional de Infectologia Evandro Chagas, Fundacao Oswaldo Cruz, Rio de Janeiro, Brazil.
⁹ Kenya Medical Research Institute/Center of Disease Control, Kisumu, Kenya.
¹⁰ Clinical HIV Research Unit, Helen Joseph Hospital, University of Witwatersrand, Johannesburg, South Africa.
¹¹ BJ Medical College Clinical Research Site, Pune, India.
¹² Moi University Clinical Research Center (MUCRC) CRS, Eldoret, Kenya.
¹³ Les Centres GHESKIO Clinical Research Site, Port-au-Prince, Haiti.
¹⁴ University of Zimbabwe Clinical Trials Research Centre, Harare, Zimbabwe.
¹⁵ Family Centre for Research with Ubuntu (FAMCRU), Stellenbosch University, Cape Town, South Africa.
¹⁶ Durban International Clinical Research Site, King Edward Hospital, Enhancing Care Foundation, Durban, South Africa.
¹⁷ Soweto AIDS Clinical Trials Group, Clinical Research Site, Perinatal HIV Research Unit, University of the Witwatersrand, Johannesburg, South Africa.
¹⁸ Barranco Clinical Research Site, Lima, Peru.
¹⁹ Research Institute for Health Sciences, Chiang Mai University, Chiang Mai, Thailand.
²⁰ San Miguel Clinical Research Site, Lima, Peru.
²¹ University of North Carolina Project, Kamazu Central Hospital, Lilongwe, Malawi.
²² Hospital Nossa Senhora da Conceicao CRS, Porto Alegre, Brazil.
²³ CART, Clinical Research Site, VHS Infection Disease Medical Centre, Chennai, India.
²⁴ Division of Infectious Diseases, University of California, San Diego, California, USA.
²⁵ Division of Infectious Diseases, Department of Medicine, University of Pittsburgh School of Medicine, Pittsburgh, Pennsylvania, USA.
²⁶ BARC-South Africa and Lancet Laboratories, Johannesburg, South Africa.
²⁷ University of Washington School of Medicine, University of Washington, Seattle, Washington, USA.

Abstract

Introduction: ACTG A5288 was a strategy trial conducted in diverse populations from multiple continents of people living with HIV (PLWH) failing second-line protease inhibitor (PI)-based antiretroviral therapy (ART) from 10 low- and middle-income countries (LMICs). Participants resistant to lopinavir (LPV) and/or multiple nucleotide reverse transcriptase inhibitors started on third-line regimens that included raltegravir (RAL), darunavir/ritonavir (DRV/r) and/or etravirine (ETR) according to their resistance profiles. At 48 weeks, 87% of these participants achieved HIV-1 RNA ≤200 copies/ml. We report here long-term outcomes over 144 weeks.

Methods: Study participants were enrolled from 2013 to 2015, prior to the availability of dolutegravir in LMICs. "Extended Follow-up" of the study started after the last participant enrolled had reached 48 weeks and included participants still on antiretroviral (ARV) regimens containing RAL, DRV/r and/or ETR at that time. RAL, DRV/r and ETR were provided for an additional 96 weeks (giving total follow-up of ≥144 weeks), with HIV-1 RNA measured at 48 and 96 weeks and CD4 count at 96 weeks after entry into Extended Follow-up. Proportion of participants with HIV-1 RNA ≤200 copies/ml was estimated every 24 weeks, using imputation if necessary to handle the different measurement schedule in Extended Follow-up; mean CD4 count changes were estimated using loess regression.

Results and discussion: Of 257 participants (38% females), at study entry, median CD4 count was 179 cells/mm³ , and HIV-1 RNA was 4.6 log₁₀ copies/ml. Median follow-up was 168 weeks (IQR: 156-204); 15 (6%) participants were lost to follow-up and 9 (4%) died. 27/246 (11%), 26/246 (11%) and 13/92 (14%) of participants who started RAL, DRV/r and ETR, respectively, discontinued these drugs; only three due to adverse events. 87%, 86%, 83% and 80% of the participants had HIV-1 RNA ≤200 copies/ml at weeks 48, 96, 144 and 168 (95% CI at week 168: 74-85%), respectively. Mean increase from study entry in CD4 count at week 168 was 265 cells/mm³ (95% CI 247-283).

Conclusions: Third-line regimens comprising of RAL, DRV/r and/or ETR were very well tolerated and had high rates of durable virologic suppression among PLWH in LMICs who were failing on second-line PI-based ART prior to the availability of dolutegravir.

Trial registration: ClinicalTrials.gov NCT01641367.

Keywords: 144 weeks efficacy; A5288; LMIC; darunavir; drug resistance; third-line ART.

Publication types

Research Support, N.I.H., Extramural

MeSH terms

Anti-HIV Agents* / therapeutic use
Anti-Retroviral Agents / therapeutic use
Darunavir / therapeutic use
Female
HIV Infections* / drug therapy
HIV Protease Inhibitors* / therapeutic use
HIV-1* / genetics
Humans
Male
Nitriles
Pyrimidines
RNA / therapeutic use
Raltegravir Potassium / adverse effects
Ritonavir / therapeutic use
Viral Load

Substances

Anti-HIV Agents
Anti-Retroviral Agents
HIV Protease Inhibitors
Nitriles
Pyrimidines
etravirine
Raltegravir Potassium
RNA
Ritonavir
Darunavir

Associated data

ClinicalTrials.gov/NCT01641367

Abstract

Publication types

MeSH terms

Substances

Associated data

Grants and funding