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PPD Global Feasibility Services
22 March 2013 Switching to Dolutegravir/Abacavir/Lamivudine Fixed Dose Combination (DTG/ABC/3TC FDC) from a PI, INI or NNRTI Based Regimen Maintains HIV Suppression at 48 Weeks J Lake,1 B Trottier,2 J Garcia-Diaz,3 H Edelstein,4 P Kumar,5 UF Bredeek,6 M Loutfy,7 C Brennan,8 J Koteff,8 B Wynne,9 J Hopking,10 M Aboud11 1University of California, Los Angeles, CA, USA; 2Clinique Médicale l‘Actuel, Montreal, QC, Canada; 3Ochsner Clinic Foundation, New Orleans, LA, USA; 4Highland Hospital, Alameda Health System, Oakland, CA, USA; 5Georgetown University, Washington, DC, USA; 6Metropolis Medical, San Francisco, CA, USA; 7Maple Leaf Research, Toronto, Ontario, Canada; 8ViiV Healthcare, Research Triangle Park, NC, USA; 9ViiV Healthcare, Collegeville, PA, USA; 10GlaxoSmithKline, London, United Kingdom; 11ViiV Healthcare, London, United Kingdom FS_Slide Deck_Kol Discussion Summary_43792_Millennium _Prostate Cancer_21 March 2013
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Introduction DTG/ABC/3TC (Triumeq) is a complete regimen built around DTG, an unboosted INSTI with a high barrier to resistance First approval of DTG/ABC/3TC: August 2014 in North America The study enrolled April 2014 to Oct 2014 STRIIVING was conducted to evaluate the efficacy, safety, tolerability, and treatment satisfaction of switching to DTG/ABC/3TC in subjects stable and suppressed on a variety of regimens T7.7 Lake et al. AIDS 2016; Durban, South Africa. Abstract THAB0203.
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STRIIVING Study Design
Countries: US, Canada, Puerto Rico Open-label, randomized 1:1 DTG/ABC/3TC 2 NRTIs + PI/r Current ARTa DTG/ABC/3TC Screening Week 24 Week 48 Primary endpoint at 24 weeks: VL <50 c/mL (Snapshot) Inclusion criteria Virologically suppressed (confirmed HIV-1 RNA <50 c/mL) HLA‑B*5701 negative Assessments CD4 cell count changes Clinical and laboratory safety Lipids, renal, bone, and cardiovascular changes Development of resistance Treatment satisfaction aStable suppressive current ART with 2 NRTIs plus either a PI, an NNRTI, or an INI. ≥40% PIs, at least 25% INIs. 90% power based on 10% non-inferiority margin (estimated response rate = 85%). Lake et al. AIDS 2016; Durban, South Africa. Abstract THAB0203.
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Study Populations Subjects randomized to DTG/ABC/3TC on Day 1 who received at least 1 dose of DTG/ABC/3TC → Early-switch Subjects randomized to continue current ART on Day 1, completed Early Switch Phase at W24, and received at least 1 dose of DTG/ABC/3TC upon switching at Week 24 → Late-switch Treatment arm Data included Early-switch Day 1 to Week 24 Day 1 to Week 48 Late-switch Week 24 to Week 48 Lake et al. AIDS 2016; Durban, South Africa. Abstract THAB0203.
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Study Disposition: Week 48
Screened (N=841) Early Switch group DTG/ABC/3TC Discontinuations: Day 1- Week 24 Day 1- Week 48 Adverse event 10 (4%) Lack of efficacy (virologic failure) Protocol deviation 15 (5%) Stopping criteria met Lost to follow-up 3 (1%) 8 (3%) Investigator discretion 5 (2%) Withdrew consent 4 (1%) 6(2%) Per sponsor request 1 (<1%) Randomized and treated DTG/ABC/3TC (n=275) Randomized and treated cART (n=278) Completed Wk 24 (N=239, 87%) Completed Wk 24 (N=245, 88%) Late Switch group DTG/ABC/3TC Discontinuations: Week 24-48 Adverse event 4 (2%) Lack of efficacy (virologic failure) Protocol deviation 1 (<1%) Stopping criteria met Lost to follow-up 3 (1%) Investigator discretion Withdrew consent 5 (2%) Late switch to DTG/ABC/3TC (N=244) Completed Wk 48 (N=230, 84%) Completed Wk 48 (N=230, 94%) Lake et al. AIDS 2016; Durban, South Africa. Abstract THAB0203.
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STRIIVING 48 Week Early Switch Arm Week 24 and 48
DTG/ABC/3TC, Day 1–Week 24 (n=275)a cART, Day 1–Week 24 (n=278)a DTG/ABC/3TC, Day 1–Week 48 (n=275) Switch to DTG/ABC/3TC , Week 24–Week 48 (n=244)b aITT-E analysis. Lake et al. AIDS 2016; Durban, South Africa. Abstract THAB0203.
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STRIIVING 48 Week Late Switch Arm 24 Weeks Post Switch
Switch to DTG/ABC/3TC , Week 24–Week 48 (n=244) Lake et al. AIDS 2016; Durban, South Africa. Abstract THAB0203.
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Week 24 and 48 Snapshot Outcomes
Early Switch Late Switch DTG/ABC/3TC N=275 n (%) Day 1 to Wk 24 Day 1 to Wk 48 N=244 n (%) Wk 24 to Wk 48 Virologic Success 233 (85) 227 (83) 224 (92) Virologic Non-response 3 (1) 1 (<1) 3 (<1) Data in window not below threshold Discontinued while VL not <50* No Virologic Data 39 (14) 47 (17) 17 (7) Discontinued due to AE or death 10 (4) 4 (2) Discontinued for other reasons 25 (9) 32 (12) 7 (3) Missing data during window but on study 4 (1) 5 (2) 6 (2) 4% of the Early Switch group discontinued treatment due to AEs at Week 24, with none between Weeks 24 and 48; 2% of the Late Switch group discontinued treatment due to AEs between Weeks 24 and 48 *Includes categories: Discontinued for lack of efficacy and Discontinued for other reason while not below threshold Lake et al. AIDS 2016; Durban, South Africa. Abstract THAB0203.
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Virologic Endpoints: DTG/ABC/3TC
No subjects met protocol-defined virologic failure in either study arm 4 subjects >50 at Week 48 window: ES (51), LS (54, 53, 156); All 4 resuppressed < 50 c/mL Early Switch Late Switch DTG/ABC/3TC N=275 Day 1 to Wk 24 Day 1 to Wk 48 N=244 Wk 24 to Wk 48 PDVFa Viral load ≥50 c/mL (snapshot) 3 (1%) 1 (<1) aSubjects with HIV-1 RNA ≥400 c/mL on 2 consecutive assessments any time after randomization are withdrawn = meets protocol defined virologic failure. Lake et al. AIDS 2016; Durban, South Africa. Abstract THAB0203.
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Adverse Events: DTG/ABC/3TC Overall Summary
Early Switch Late Switch DTG/ABC/3TC N=275 n (%) Day 1 to Wk 24 Day 1 to Wk 48 N=244 n (%) Wk 24 to Wk 48 Any adverse event, n (%) 180 (65) 206 (75) 146 (60) Any drug-related event (occurring ≥2% of subjects in either arm) 57 (21) 60 (22) 32 (13) Nausea 20 (7) 9 (4) Diarrhea 9 (3) 3 (1) Fatigue Headache 7 (3) 6 (2) Insomnia 5 (2) Dizziness 2 (<1) Abnormal dreams 4 (1) Any serious eventa Any fatal eventa 1 (<1) Discontinuations due to AE or death 10 (4) 4 (2) . aNone were considered drug-related events. Lake et al. AIDS 2016; Durban, South Africa. Abstract THAB0203.
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Common Adverse Events: DTG/ABC/3TC (≥5% in Any Treatment)
Early Switch Late Switch DTG/ABC/3TC N=275 n (%) Day 1 to Wk 24 Day 1 to Wk 48 N=244 n (%) Wk 24 to Wk 48 Nausea 27 (10) 28 (10) 15 (6) Upper respiratory tract infection 20 (7) 35 (13) 22 (9) Diarrhea 9 (4) Fatigue 19 (7) 22 (8) 6 (2) Headache 13 (5) 17 (6) 10 (4) Cough 14 (5) Insomnia Nasopharyngitis Lake et al. AIDS 2016; Durban, South Africa. Abstract THAB0203.
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Conclusions Efficacy The virologic response rate was maintained through 48 weeks in the Early Switch group In the Late Switch group, virologic suppression was observed in 92% of subjects on DTG/ABC/3TC (24 weeks post-switch) There were no PDVFs in the study Tolerability There were no further discontinuations due to AEs in the Early Switch arm post-Week 24 Low rates of discontinuations in the Late Switch arm (2%) Summary Data through 48 weeks support switching to DTG/ABC/3TC once daily for HIV‑1 subjects on stable suppressive cART Lake et al. AIDS 2016; Durban, South Africa. Abstract THAB0203.
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