Affiliation:
1. Department of Medicine, Command Hospital Lucknow, 226002, India
2. Department of Medicine, Army College of
Medical Sciences, New Delhi, 110010, India
3. Department of Surgery, Army College of Medical Sciences, New Delhi,
110010, India
4. Army Base Hospital, New Delhi, 110010, India
5. Department of Clinical Research, PLUM Ltd., New
Delhi, 110008, India.
Abstract
Background:
Dolutegravir (DTG) is a novel yet preferential first-and-second-line treatment
for persons living with HIV (PLH). Owing to its recent introduction, DTG-based regimens
have not undergone a comprehensive, systematic evaluation regarding their real-world utilization
and safety profile among a sizeable Indian population.
Objective:
This study aimed to assess the 24-week immunovirological outcomes, anthropometric
and metabolic changes, tolerability, and adverse events (AEs) of DTG-based antiretroviral (ART)
regimens.
Methods:
A single-centre phase-IV non-interventional observational study involving 322 ART--
naïve and treatment-experienced PLH initiating DTG-based-regimens until October 2022 were followed
up for outcomes at 24 weeks.
Results:
At 24 weeks, all PLH (n=113) in the naïve group, all PLH (n=67) in the first-line substitution
group, 93.9% PLH (n=46) in the first-line failure group, and 95.7% PLH (n=89) in the second-
line substitution group were virologically suppressed to plasma HIV-RNA <1000
copies/mL. Virological suppression rates to plasma HIV-RNA <200 copies/mL and <50
copies/mL were consistent among PLH who received DTG as first- or second-line ART.
The mean-unadjusted weight gain observed was 3.5 kg (SE: 0.330), and it was significantly higher
in PLH with poorer health at baseline (either HIV-RNA ≥ 1000 copies/ml or CD4 cell count
<350 cells/μL). Overall, 27.3% PLH (n=88) gained ≥10% of their baseline body weight, corresponding
to 3.7% incidence (n=10) of treatment-emergent clinical obesity [1]. DTG had an overall
lipid-neutral effect, with an advantageous effect being observed in PLH switching from non-nucleoside
analogue reverse-transcriptase inhibitors (NNRTI) or ritonavir-boosted protease inhibitors
(b/PI), especially in dyslipidemic pre-treated PLH (median change in total cholesterol: 28.5
mg/dL and triglycerides: 51 mg/dL), possibly emanating from the withdrawal of the offending
ART. The incidence of DTG-specific AEs, including CNS AEs, was low. Two PLH developed
proximal myopathy and one developed transaminitis, warranting DTG discontinuation. Asymptomatic
serum-CPK elevation and drug-induced transaminitis were seen in 25.2% (n=27) and 3.2%
(n=10) PLH, respectively. No apparent negative effects on renal function were detected.
Results:
At 24 weeks, all PLH (n = 113) in the naïve group, all PLH (n = 67) in the first-line substitution
group, 93.9% PLH (n = 46) in the first-line failure group, and 95.7% PLH (n = 89) in the
second-line substitution group were virologically suppressed to plasma HIV-RNA <1000
copies/mL. Virological suppression rates to plasma HIV-RNA <200 copies/mL and <50
copies/mL were consistent among PLH who received DTG as first- or second-line ART.
:
The mean-unadjusted weight gain observed was 3.5 kg (SE: 0.330), and it was significantly higher
in PLH with poorer health at baseline (either HIV-RNA ≥ 1000 copies/ml or CD4 cell count
<350 cells/μL). Overall, 27.3% PLH (n = 88) gained ≥10% of their baseline body weight, corresponding
to 3.7% incidence (n = 12) of treatment-emergent clinical obesity. DTG had an overall
lipid-neutral effect, with an advantageous effect being observed in PLH switching from non-nucleoside
analogue reverse-transcriptase inhibitors (NNRTI) or ritonavir-boosted protease inhibitors
(b/PI), especially in dyslipidemic pre-treated PLH (median change in total cholesterol: 28.5
mg/dL and triglycerides: 51 mg/dL), possibly emanating from the withdrawal of the offending
ART. The incidence of DTG-specific AEs, including CNS AEs, was low. Two PLH developed
proximal myopathy and one developed transaminitis, warranting DTG discontinuation. Asymptomatic
serum-CPK elevation and drug-induced transaminitis were seen in 25.2% (n = 27) and 3.2%
(n = 10) PLH, respectively. No apparent negative effects on renal function were detected.
Conclusion:
Our results from a large Indian cohort indicate a favourable virological and
metabolic response, with good tolerance of DTG-based ART at 24 weeks.
Publisher
Bentham Science Publishers Ltd.
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