Open Access
Open access
Journal of the International AIDS Society, volume 28, issue 2

Pharmacokinetics, safety and efficacy of elvitegravir/cobicistat/emtricitabine/tenofovir alafenamide in children with HIV aged from 2 years and weighing at least 14 kg

Eva Natukunda 1
Aditya H. Gaur 2
Pope Kosalaraksa 3
Elizabeth Hellström 4
Renate Strehlau 5
Afaaf Liberty 6
Stephanie Cox 7
Rory Leisegang 7
Ramesh Palaparthy 7
Susanne Crowe 7
Vinicius Vieira 7
Kathryn Kersey 7
Natella Rakhmanina 8, 9, 10
Show full list: 13 authors
1
 
Department of Paediatrics Joint Clinical Research Centre Kampala Uganda
2
 
3
 
4
 
Be Part Yoluntu Centre Paarl South Africa
5
 
6
 
Chris Hani Baragwanath Hospital Johannesburg South Africa
7
 
Gilead Sciences, Inc. Foster City California USA
8
 
9
 
10
 
Elizabeth Glaser Pediatric AIDS Foundation Washington DC USA
Publication typeJournal Article
Publication date2025-01-30
scimago Q1
SJR1.934
CiteScore8.6
Impact factor4.6
ISSN17582652
Abstract
Introduction

Elvitegravir/cobicistat/emtricitabine/tenofovir alafenamide (E/C/F/TAF) was efficacious and well tolerated in children/adolescents with HIV (aged ≥6 years, weighing ≥25 kg) in a Phase 2/3 study. Here, we report data from children aged ≥2 years and weighing ≥14–<25 kg.

Methods

This is an analysis of data from the youngest cohort in an open‐label, multicentre, multi‐cohort, single‐group, international study of children/adolescents with HIV. Participants in this cohort were children aged ≥2 years, weighing ≥14–<25 kg at screening and able to swallow tablets, on stable antiretroviral therapy with virologic suppression (HIV‐1 RNA <50 copies/ml for ≥6 consecutive months) and a CD4 count ≥400 cells/µl. Eligible participants received low‐dose E/C/F/TAF (90/90/120/6 mg) once daily through Week 48. The study included pharmacokinetic evaluation of the low‐dose E/C/F/TAF tablet at Week 2. Safety, efficacy, palatability and acceptability were also evaluated.

Results

Between 16 January and 25 November 2019, 27 participants were enrolled with a median (quartile [Q]1, Q3) age of 6 (4, 8) years, body weight of 19.3 (17.0, 20.5) kg, CD4 count of 1061 (895, 1315) cells/µl and CD4 cell percentage of 37.4 (30.6, 40.3). Most (92.6%) participants acquired HIV through vertical transmission. On 6 October 2020 (data‐cut), median (Q1, Q3) exposure to E/C/F/TAF was 48.3 (48.0, 60.1) weeks. Pharmacokinetic parameters were within the safe and efficacious range of previous data in adult and paediatric populations. Drug‐related treatment‐emergent adverse events occurred in 4/27 (15%) participants. There were no Grade 3/4 adverse events, or adverse events leading to E/C/F/TAF discontinuation. One participant experienced a serious treatment‐emergent adverse event (Grade 2 pneumonia not considered E/C/F/TAF related). Virologic suppression (US FDA Snapshot algorithm) was maintained by 26/27 (96%) participants at Weeks 24 and 48. At Week 48, most children reported positive palatability (84.6%) and acceptability (96.2%).

Conclusions

These data support the use of single‐tablet E/C/F/TAF (90/90/120/6 mg) regimen for the treatment of HIV in children aged ≥2 years and weighing ≥14–<25 kg.

Clinical Trial Number

NCT01854775

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