Lopinavir/ritonavir monotherapy after 24 weeks of second-line antiretroviral therapy in Africa: a randomized controlled trial (SARA)

Charles F Gilks; A Sarah Walker; David T Dunn; Diana M Gibb; Ben Kikaire; Andrew Reid; Hellen Musana; Ivan Mambule; Ronnie Kasirye; Val Robertson; Francis Ssali; Moira Spyer; Deenan Pillay; David Yirrell; Pontiano Kaleebu; DART Virology Group and Trial Team

doi:10.3851/IMP2253

Lopinavir/ritonavir monotherapy after 24 weeks of second-line antiretroviral therapy in Africa: a randomized controlled trial (SARA)

Antivir Ther. 2012;17(7):1363-73. doi: 10.3851/IMP2253. Epub 2012 Jul 19.

Authors

Charles F Gilks¹, A Sarah Walker, David T Dunn, Diana M Gibb, Ben Kikaire, Andrew Reid, Hellen Musana, Ivan Mambule, Ronnie Kasirye, Val Robertson, Francis Ssali, Moira Spyer, Deenan Pillay, David Yirrell, Pontiano Kaleebu; DART Virology Group and Trial Team

Collaborators

DART Virology Group and Trial Team:
P Kaleebu, D Pillay, V Robertson, D Yirrell, S Tugume, M Chirara, P Katundu, F Lyagoba, D Dunn, R Goodall, A McCormick, M Spyer, J Nkalubo, P Hughes, C Gilks, D M Gibb, C Parry, A Kapaata, B Magambo M Nabankkema, P Nkurunziza, M Katuramur, P Awio, T Musunga, H Grosskurth, P Munderi, G Kabuye, D Nsibambi, R Kasirye, E Zalwango, M Nakazibwe, B Kikaire, G Nassuna, R Massa, K Fadhiru, M Namyalo, A Zalwango, L Generous, P Khauka, N Rutikarayo, W Nakahima, A Mugisha, J Todd, J Levin, S Muyingo, A Ruberantwari, P Kaleebu, D Yirrell, N Ndembi, F Lyagoba, P Hughes, M Aber, A Medina Lara, S Foster, J Amurwon, B Nyanzi Wakholi, J Whitworth, K Wangati, B Amuron, D Kajungu, J Nakiyingi, W Omony, K Fadhiru, D Nsibambi, P Khauka, P Mugyenyi, C Kityo, F Ssali, D Tumukunde, T Otim, J Kabanda, H Musana, J Akao, H Kyomugisha, A Byamukama, J Sabiiti, J Komugyena, P Wavamunno, S Mukiibi, A Drasiku, R Byaruhanga, O Labeja, P Katundu, S Tugume, P Awio, A Namazzi, G T Bakeinyaga, H Katabira, D Abaine, J Tukamushaba, W Anywar, W Ojiambo, E Angweng, S Murungi, W Haguma, S Atwiine, J Kigozi, L Namale, A Mukose, G Mulindwa, D Atwiine, A Muhwezi, E Nimwesiga, G Barungi, J Takubwa, S Murungi, D Mwebesa, G Kagina, M Mulindwa, F Ahimbisibwe, P Mwesigwa, S Akuma, C Zawedde, D Nyiraguhirwa, C Tumusiime, L Bagaya, W Namara, J Kigozi, J Karungi, R Kankunda, R Enzama, A Latif, J Hakim, V Robertson, A Reid, E Chidziva, R Bulaya-Tembo, G Musoro, F Taziwa, C Chimbetete, L Chakonza, A Mawora, C Muvirimi, G Tinago, P Svovanapasis, M Simango, O Chirema, J Machingura, S Mutsai, M Phiri, T Bafana, M Chirara, L Muchabaiwa, M Muzambi, J Mutowo, T Chivhunga, E Chigwedere, M Pascoe, C Warambwa, E Zengeza, F Mapinge, S Makota, A Jamu, N Ngorima, H Chirairo, S Chitsungo, J Chimanzi, C Mawen, R Warara, M Matongo, S Mudzingwa, M Jangano, K Moyo, L Vere, N Mdege, I Machingura, E Katabira, A Ronald, A Kambungu, F Lutwama, I Mambule, A Nanfuka, J Walusimbi, E Nabankema, R Nalumenya, T Namuli, R Kulume, I Namata, L Nyachwo, A Florence, A Kusiima, E Lubwama, R Nairuba, F Oketta, E Buluma, R Waita, H Ojiambo, F Sadik, J Wanyama, P Nabongo, J Oyugi, F Sematala, A Muganzi, C Twijukye, H Byakwaga, R Ochai, D Muhweezi, A Coutinho, B Etukoit, C Gilks, K Boocock, C Puddephatt, C Grundy, J Bohannon, D Winogron, D M Gibb, A Burke, D Bray, A Babiker, A S Walker, H Wilkes, M Rauchenberger, S Sheehan, C Spencer-Drake, K Taylor, M Spyer, A Ferrier, B Naidoo, D Dunn, R Goodall, J H Darbyshire, L Peto, R Nanfuka, C Mufuka-Kapuya, A Medina Lara, S Foster, J Amurwon, B Nyanzi Wakholi, J Kigozi, L Muchabaiwa, M Muzambi, I Weller, A Babiker, S Bahendeka, M Bassett, A Chogo Wapakhabulo, J H Darbyshire, B Gazzard, C Gilks, H Grosskurth, J Hakim, A Latif, C Mapuchere, O Mugurungi, P Mugyenyi, C Burke, S Jones, C Newland, G Pearce, S Rahim, J Rooney, M Smith, W Snowden, J-M Steens, A Breckenridge, A McLaren, C Hill, J Matenga, A Pozniak, D Serwadda, T Peto, A Palfreeman, M Borok, E Katabira

Affiliation

¹ Imperial College, London, UK. gilksc@unaids.org

PMID: 22814125
DOI: 10.3851/IMP2253

Abstract

Background: Boosted protease inhibitor (bPI) monotherapy (bPImono) potentially has substantial cost, safety and operational benefits. It has never been evaluated as second-line antiretroviral therapy (ART) in Africa.

Methods: After 24 weeks of lopinavir/ritonavir-containing second-line therapy, DART participants were randomized to remain on combination therapy (CT), or change to bPImono maintenance (SARA trial; ISRCTN53817258). Joint primary end points were CD4(+) T-cell changes 24 weeks later and serious adverse events (SAEs); retrospectively assayed viral load (VL) was a secondary end point. Analyses were intention-to-treat.

Results: A total of 192 participants were randomized to CT (n=95) or bPImono (n=97) and followed for median 60 weeks (IQR 45-84). Participants received median 4.0 years (IQR 3.5-4.4) first-line ART. Median CD4(+) T-cell count at first-line failure was 86 cells/mm(3) (47-136), increasing to 245 cells/mm(3) (173-325) after 24-week induction when 77% had VL<50 copies/ml. Overall, 44 (23%) were receiving second-line therapy with bPI and nucleoside reverse transcriptase inhibitors (NRTI) only, and 148 (77%) with bPI plus non-NRTI (NNRTI) with or without NRTI. At 24 weeks after randomization to CT versus bPImono, mean CD4(+) T-cell increase was 42 (CT, n=85) versus 49 cells/mm(3) (bPImono, n=88; adjusted difference 13 [95% CI -15, 43], P=0.37; non-inferior compared with predetermined non-inferiority margin [-33]). Virological suppression was greater for CT versus bPImono (trend P=0.009): 77% (70/91) versus 60% (56/94) were <50 copies/ml, and 5% (5) versus 14% (13) were ≥1,000 copies/ml, respectively. A total of 0 (0%) versus 5 (5%) participants had major protease inhibitor mutations and 3 (3%) versus 0 (0%) new NNRTI/NRTI mutations were detected during follow-up. Two participants (1 CT and 1 bPImono) died >24 weeks after randomization, and 5 (2 CT and 3 bPImono) experienced SAEs (P=0.51).

Conclusions: bPImono following a 24-week second-line induction was associated with similar CD4(+) T-cell response, but increased low-level viraemia, generally without protease inhibitor resistance. Longer-term trials are needed to provide definitive evidence about effectiveness in Africa.

Publication types

Randomized Controlled Trial
Research Support, Non-U.S. Gov't

MeSH terms

Adult
Africa
CD4 Lymphocyte Count
Drug Resistance, Viral
Drug Therapy, Combination
Female
HIV / pathogenicity
HIV Infections / drug therapy*
HIV Infections / pathology
HIV Infections / virology
HIV Protease Inhibitors / adverse effects
HIV Protease Inhibitors / therapeutic use*
Humans
Lopinavir / adverse effects
Lopinavir / therapeutic use*
Male
Middle Aged
Mutation
RNA, Viral / blood
Ritonavir / adverse effects
Ritonavir / therapeutic use*
Time Factors
Treatment Outcome
Viral Load
Viremia / pathology
Viremia / virology

Substances

HIV Protease Inhibitors
RNA, Viral
Lopinavir
Ritonavir

Abstract

Publication types

MeSH terms

Substances

Grants and funding