304777
Switch from NNRTI plus TVD to STB Maintains HIV Suppression and is Well- Tolerated
Methods: Subjects suppressed on NNRTI + TVD for ≥ 6 months were randomized (2:1) to switch to STB or remain on their regimen. Eligibility criteria included CrCl ≥ 70 mL/min, no resistance to FTC and TDF, exposure ≤2 prior ARV regimens and no history of virologic failure. Primary endpoint was the proportion of subjects who maintained HIV-1 RNA < 50 c/mL at W48 by FDA snapshot.
Results: 434 subjects were randomized and treated (291 STB; 143 NNRTI). Baseline characteristics were similar between the two groups. STB was noninferior to NNRTI regimens, as 93% and 88% respectively maintained HIV-1 RNA < 50 c/mL at W48 (difference 5.3%, 95% CI -0.5%, +12.0%). Virologic failure rates were 1% with no resistance detected in either group. Mild and transient headache and nausea occurred at slightly higher rates in the STB than NNRTI group. Grade 3 or 4 adverse events were low and similar in both groups. Median changes in CrCl (mL/min) at W48 were -11.6 and -0.2 respectively. Subjects who switched to STB reported lower rates of neuropsychiatric symptoms compared to baseline and to those remaining on NNRTI. They also reported more treatment satisfaction.
Conclusions: Switching to STB was associated with high rates of virologic suppression, no resistance development, favorable tolerability, and improved treatment satisfaction.
Learning Areas:
Basic medical science applied in public healthChronic disease management and prevention
Other professions or practice related to public health
Provision of health care to the public
Learning Objectives:
Describe the efficacy, safety and patient benefits of switching from a NNRTI-based regimen to the single-tablet-regimen of STRIBILD (STB) in pts with HIV-1 infection.
Keyword(s): HIV/AIDS, Treatment
Organization/institution whose products or services will be discussed: STB does not currently have a "switch" indication in the FDA label, however this data is being submitted now to request this label change.
Qualified on the content I am responsible for because: I was a study investigator for this study "121," aka the switch from NNRTI plus TVD to Stribild. I have over 16 years practicing medicine with specialty training in infectious diseases, especially HIV medicine. I am certified by the American Academy of HIV Medicine and I have given numerous talks at international conferences on HIV.
Any relevant financial relationships? Yes
Name of Organization | Clinical/Research Area | Type of relationship |
---|---|---|
Gilead Sciences | HIV | Advisory Committee/Board, Consultant, Speaker's bureau and teaching engagements and Stock Ownership |
Abbott/AbbVie | HIV | Advisory Committee/Board and Consultant |
ViiV | HIV | Advisory Committee/Board, Consultant and Speaker's bureau and teaching engagements |
Bristol-Myers Squibb | HIV | Advisory Committee/Board and Consultant |
I agree to comply with the American Public Health Association Conflict of Interest and Commercial Support Guidelines, and to disclose to the participants any off-label or experimental uses of a commercial product or service discussed in my presentation.