Analytical treatment interruption among women with HIV in southern Africa who received VRC01 or placebo in the Antibody Mediated Prevention Study : ATI stakeholder engagement, implementation and early clinical data
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Publisher
Wiley
Abstract
INTRODUCTION : Antiretroviral therapy (ART) prevents and treats, but does not eradicate, HIV. Early ART initiation is associated with post-ART virologic control, particularly among African women, and anti-HIV-1 broadly neutralizing antibodies (bnAbs) may modulate immune responses to HIV. We evaluate whether early ART with or without anti-HIV-1 bnAb VRC01, present at HIV acquisition, is associated with later ART-free control in African women and we assess potential associations with observed control.
METHODS : Stakeholder engagement informed analytical treatment interruption (ATI) study design and implementation. Participants who received placebo or VRC01 and acquired HIV in the Antibody Mediated Prevention efficacy trial were assessed for ATI eligibility, including HIV acquisition within 8 weeks of receiving VRC01 or placebo, followed by early ART initiation and ≥1 year of viral suppression. Participation facilitators and barriers were assessed. From May 2021 to February 2024, participants enrolled, stopped ART and received frequent viral load and CD4+ T-cell count monitoring for safety and assessment of meeting ART reinitiation criteria.
RESULTS : Thirteen women enrolled from southern Africa. No ATI-related serious adverse events (AEs), HIV transmissions, pregnancies or ≥Grade 2 AEs were observed. Eight sexually transmitted infections were diagnosed in seven women during ATI. Two participants had tenofovir levels consistent with use during ATI; 2/11 (18%) who completed ATI without antiretroviral use exhibited ART-free control for ≥32 weeks. The median time to confirmed VL≥200 was 5.4 weeks (range 2.7−112). The most common ART reinitiation criterion met was virologic (n = 7). VRC01 receipt proximate to HIV acquisition was not associated with control. Controllers versus non-controllers did not differ by early post-acquisition viral load kinetics, acquired virus characteristics, or time from estimated acquisition to closest infusion or to ART initiation.
CONCLUSIONS : In a safe, well-tolerated ATI, 18% of 11 African women exhibited post-intervention control. Design and implementation lessons inform future ATIs in Africa. Analyses of peri-acquisition and post-ATI host and viral characteristics can inform the development of interventions for HIV cure, prevention and treatment.
CLINICAL TRIAL REGISTRATION : NCT04860323
Description
DATA AVAILABILITY STATEMENT : The data generated in this study are provided at https://dataverse.harvard.edu/dataverse/hvtn805-hptn093. All individual participant data have been de-identified.
SUPPLEMENTARY FIGURES : FIGURE S1. Viral Load Metrics. (A) First positive viral load observed in the parent AMP trial HVTN 703/HPTN 081. Model estimated metrics (B) set point, (C) peak and (D) 3-month average, based on pre-ART viral load data from the parent AMP trial [59]. Two participants with DBS ARV levels consistent with ongoing ARV use during ATI are excluded from this analysis. Participant 805-131856 (indicated with *) did not have enough data to fit the models in B–D. Filled squares indicate controller, open squares indicate non-controller. Placebo (black), VRC01 30 mg/kg (dark purple) and VRC01 10 mg/kg (light purple). FIGURE S2. IC80 values of primary viral isolates. (A) Epitope Distance (B) Physicochemical distance (C) Geometric mean IC80 was right censored at 100 µg/ml. Two participants with DBS ARV levels consistent with ongoing ARV use during ATI are excluded from this analysis. Participants 805-861376, 805-907560, 805-370244, 805-131856, and 805-266234 each had two primary viral isolates. The two isolates for 805-861378 indicated with * have values ≥100. Metrics in panels A and B are from [60] and C is from [49]. Filled squares indicate controller, open squares indicate non-controller. Placebo (black), VRC01 30 mg/kg (dark purple) and VRC01 10 mg/kg (light purple).
SUPPLEMENTARY FIGURES : FIGURE S1. Viral Load Metrics. (A) First positive viral load observed in the parent AMP trial HVTN 703/HPTN 081. Model estimated metrics (B) set point, (C) peak and (D) 3-month average, based on pre-ART viral load data from the parent AMP trial [59]. Two participants with DBS ARV levels consistent with ongoing ARV use during ATI are excluded from this analysis. Participant 805-131856 (indicated with *) did not have enough data to fit the models in B–D. Filled squares indicate controller, open squares indicate non-controller. Placebo (black), VRC01 30 mg/kg (dark purple) and VRC01 10 mg/kg (light purple). FIGURE S2. IC80 values of primary viral isolates. (A) Epitope Distance (B) Physicochemical distance (C) Geometric mean IC80 was right censored at 100 µg/ml. Two participants with DBS ARV levels consistent with ongoing ARV use during ATI are excluded from this analysis. Participants 805-861376, 805-907560, 805-370244, 805-131856, and 805-266234 each had two primary viral isolates. The two isolates for 805-861378 indicated with * have values ≥100. Metrics in panels A and B are from [60] and C is from [49]. Filled squares indicate controller, open squares indicate non-controller. Placebo (black), VRC01 30 mg/kg (dark purple) and VRC01 10 mg/kg (light purple).
Keywords
Antiretroviral therapy (ART), Broadly neutralizing antibodies (bnAbs), Analytical treatment interruption (ATI), Human immunodeficiency virus (HIV), HIV remission, HIV cure, Stakeholder engagement, People living with HIV (PLHIV)
Sustainable Development Goals
SDG-03: Good health and well-being
Citation
Karuna, S., Laher, F., Dadabhai, S. et al. 2025, 'Analytical treatment interruption among women with HIV in southern Africa who received VRC01 or placebo in the Antibody Mediated Prevention Study: ATI stakeholder engagement, implementation and early clinical data', Journal of the International AIDS Society, vol. 28, no. 6, art. e26495, pp. 1-15, doi : 10.1002/jia2.26495.