Clinical and programmatic outcomes of HIV-exposed infants enrolled in care at geographically diverse clinics, 1997-2021: A cohort study Public Deposited

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  • Edmonds, A.
    • Affiliation: Gillings School of Global Public Health, Department of Epidemiology
  • Brazier, E.
    • Other Affiliation: City University of New York
  • Musick, B.S.
    • Other Affiliation: Indiana University, Indianapolis
  • Yotebieng, M.
    • Other Affiliation: Albert Einstein College of Medicine
  • Humphrey, J.
    • Other Affiliation: Indiana University, Indianapolis
  • Abuogi, L.L.
    • Other Affiliation: University of Colorado
  • Adedimeji, A.
    • Other Affiliation: Albert Einstein College of Medicine
  • Keiser, O.
    • Other Affiliation: University of Geneva
  • Msukwa, M.
    • Other Affiliation: University of Maryland
  • Carlucci, J.G.
    • Other Affiliation: Indiana University, Indianapolis
  • Maia, M.
    • Other Affiliation: Federal University of Minas Gerais
  • Pinto, J.A.l
    • Other Affiliation: Federal University of Minas Gerais
  • Leroy, V.
    • Other Affiliation: Université de Toulouse
  • Davies, M.-A.
    • Other Affiliation: University of Cape Town
  • Wools-Kaloustian, K.K.
    • Other Affiliation: Indiana University, Indianapolis
Abstract
  • Background Although 1.3 million women with HIV give birth annually, care and outcomes for HIVexposed infants remain incompletely understood. We analyzed programmatic and health indicators in a large, multidecade global dataset of linked mother-infant records from clinics and programs associated with the International epidemiology Databases to Evaluate AIDS (IeDEA) consortium. Methods and findings HIV-exposed infants were eligible for this retrospective cohort analysis if enrolled at <18 months at 198 clinics in 10 countries across 5 IeDEA regions: East Africa (EA), Central Africa (CA), West Africa (WA), Southern Africa (SA), and the Caribbean, Central, and South America network (CCASAnet). We estimated cumulative incidences of DNA PCR testing, loss to follow-up (LTFU), HIV diagnosis, and death through 24 months of age using proportional subdistribution hazard models accounting for competing risks. Competing risks were transfer, care withdrawal, and confirmation of negative HIV status, along with LTFU and death, when not the outcome of interest. In CA and EA, we quantified associations between maternal/infant characteristics and each outcome. A total of 82,067 infants (47,300 EA, 10,699 CA, 6,503 WA, 15,770 SA, 1,795 CCASAnet) born from 1997 to 2021 were included. Maternal antiretroviral therapy (ART) use during pregnancy ranged from 65.6% (CCASAnet) to 89.5% (EA), with improvements in all regions over time. Twenty-four-month cumulative incidences varied widely across regions, ranging from 12.3% (95% confidence limit [CL], 11.2%,13.5%) in WA to 94.8% (95% CL, 94.6%,95.1%) in EA for DNA PCR testing; 56.2% (95% CL, 55.2%,57.1%) in EA to 98.5% (95% CL, 98.3%,98.7%) in WA for LTFU; 1.9% (95% CL, 1.6%,2.3%) in WA to 10.3% (95% CL, 9.7%,10.9%) in EA for HIV diagnosis; and 0.5% (95% CL, 0.2%,1.0%) in CCASAnet to 4.7% (95% CL, 4.4%,5.0%) in EA for death. Although infant retention did not improve, HIV diagnosis and death decreased over time, and in EA, the cumulative incidence of HIV diagnosis decreased substantially, declining to 2.9% (95% CL, 1.5%,5.4%) in 2020. Maternal ART was associated with decreased infant mortality (subdistribution hazard ratio [sdHR], 0.65; 95% CL, 0.47,0.91 in EA, and sdHR, 0.51; 95% CL, 0.36,0.74 in CA) and HIV diagnosis (sdHR, 0.40; 95% CL, 0.31,0.50 in EA, and sdHR, 0.41; 95% CL, 0.31,0.54 in CA). Study limitations include potential misclassification of outcomes in real-world service delivery data and possible nonrepresentativeness of IeDEA sites and the population of HIV-exposed infants they serve. Conclusions While there was marked regional and temporal heterogeneity in clinical and programmatic outcomes, infant LTFU was high across all regions and time periods. Further efforts are needed to keep HIV-exposed infants in care to receive essential services to reduce HIV infection and mortality.
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  • Attribution 4.0 International
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  • PLoS Medicine
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  • 19
Journal issue
  • 9
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  • English
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