Switch to Stribild versus continuation of NVP or RPV with FTC and TDF in virologically suppressed HIV adults: a STRATEGY-NNRTI subgroup analysis

Hans-Juergen Stellbrink; Andrea Antinori; Anton Pozniak; Jason Flamm; Fritz Bredeek; Kiran Patel; Will Garner; David Piontkowsky

doi:10.7448/IAS.17.4.19793

Switch to Stribild versus continuation of NVP or RPV with FTC and TDF in virologically suppressed HIV adults: a STRATEGY-NNRTI subgroup analysis

J Int AIDS Soc. 2014 Nov 2;17(4 Suppl 3):19793. doi: 10.7448/IAS.17.4.19793. eCollection 2014.

Authors

Hans-Juergen Stellbrink¹, Andrea Antinori², Anton Pozniak³, Jason Flamm⁴, Fritz Bredeek⁵, Kiran Patel⁶, Will Garner⁶, David Piontkowsky⁶

Affiliations

¹ Infectious Diseases, ICH Study Center, Hamburg, Germany.
² Infectious Diseases, Istituto Nazionale Malattie Infettive Lazzaro Spallanzani IRCCS, Rome, Italy.
³ HIV Unit, St Stephens Centre, Chelsea and Westminster Hospital, London, UK.
⁴ Infectious Diseases, Kaiser Permanente, Sacramento, CA, USA.
⁵ HIV Medicine, Metropolis Medical Group, San Francisco, CA, USA.
⁶ HIV Division, Gilead Sciences, Foster City, CA, USA.

Abstract

Introduction: Switch to Stribild (STB) was non-inferior to continuation of a non-nucleoside reverse transcriptase inhibitor (NNRTI) with emtricitabine and tenofovir DF (FTC/TDF) at week 48 in virologically suppressed HIV adults (1). We report the Week 48 efficacy and safety of STB versus nevirapine (NVP) or rilpivirine (RPV) with FTC/TDF in suppressed subjects.

Materials and methods: Virologically suppressed subjects on an NNRTI with FTC/TDF regimens for ≥6 months were randomized (2:1) to switch to STB versus continue their NNRTI regimen. Eligibility criteria included no documented resistance to FTC and TDF, no history of virologic failure and eGFR ≥70 mL/min. The primary endpoint was the proportion of subjects in the modified ITT population who maintained HIV-1 RNA <50 copies(c)/mL at Week 48 by FDA snapshot algorithm (12% non-inferiority margin). Subgroup analysis by non-EFV NNRTI use (NVP [74]; RPV [19]; etravirine [3]) at screening was pre-specified.

Results: The mITT population included 433 subjects who were randomized and treated. In the non-EFV NNRTI subgroup, 59 switched to STB; 37 continued a non-EFV NNRTI (27 NVP, 10 RPV) with FTC/TDF. At week 48, 97% STB versus 95% non-EFV NNRTI maintained HIV-1 RNA <50 c/mL. No emergent resistance was detected in either group. No difference in median increases from baseline in CD4 count at week 48 (cells/µL): 25 STB versus 55 non-EFV NNRTI (p=0.78). No discontinuation due to adverse events; no cases of proximal renal tubulopathy. As expected, there were no significant changes in the frequency of neuropsychiatric symptoms (i.e. anxiety, insomnia, dizziness, vivid dreams, weird/intense dreams, and nightmares) reported on the HIV Symptom Index at week 48 compared to baseline after switching to STB. There was a greater but non-progressive decrease from baseline in eGFR in the STB versus non-EFV NNRTI group; median changes (mL/min) at week 48: -9.1 versus -1.4. Switch to STB was associated with a higher treatment ease (convenience, flexibility, demand, lifestyle, understanding) score (range: -15 to 15) at week 4 (median: 14 vs 11; p=0.047) and week 24 (median: 14 vs 12.5; p=0.038).

Conclusions: In this small group of virologically suppressed subjects, switch to STB vs continuation of NVP or RPV with FTC/TDF was safe, well-tolerated, and associated with a high rate of virologic suppression at week 48. There was more treatment ease with STB use.