Abstract

The ZVITAMBO trial recruited 14,110 mother–infant pairs to a randomized controlled trial of vitamin A between 1997 and 2000, before the availability of antiretroviral therapy for HIV prophylaxis or treatment in Zimbabwe. The HIV status of mothers and infants was well characterized through 1–2 years of follow-up, leading to the largest cohort to date of HIV-exposed uninfected (HEU) infants (n = 3135), with a suitable comparison group of HIV-unexposed infants (n = 9510). Here, we draw on 10 years of published findings from the ZVITAMBO trial. HEU infants had increased morbidity compared to HIV-unexposed infants, with 50% more hospitalizations in the neonatal period and 30% more sick clinic visits during infancy, particularly for skin infections, lower respiratory tract infections, and oral thrush. HEU children had 3.9-fold and 2.0-fold higher mortality than HIV-unexposed children during the first and second years of life, respectively, most commonly due to acute respiratory infections, diarrhea/dysentery, malnutrition, sepsis, and meningitis. Infant morbidity and mortality were strongly related to maternal HIV disease severity, and increased morbidity remained until maternal CD4 counts were >800 cells/μL. HEU infants were more likely to be premature and small-for-gestational age than HIV-unexposed infants, and had more postnatal growth failure. Here, we propose a conceptual framework to explain the increased risk of infectious morbidity, mortality, and growth failure among HEU infants, hypothesizing that immune activation and inflammation are key drivers of both infection susceptibility and growth failure. Future studies should further dissect the causes of infection susceptibility and growth failure and determine the impact of ART and cotrimoxazole on outcomes of this vulnerable group of infants in the current era.

Highlights

  • Before the availability of antiretroviral therapy (ART), around a quarter of infants born to HIVinfected women in Zimbabwe acquired the infection [1] and almost two-thirds of perinatally infected children died before their second birthday [2]

  • Hospitalization was 50% more frequent among HIV-exposed uninfected (HEU) infants in the first month of life, and mortality rates were higher over the 24-month follow-up period

  • HEU infants were at higher risk of stunting, wasting, and underweight than HIV-unexposed infants, maternal disease severity was not associated with growth outcomes

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Summary

INTRODUCTION

Before the availability of antiretroviral therapy (ART), around a quarter of infants born to HIVinfected women in Zimbabwe acquired the infection [1] and almost two-thirds of perinatally infected children died before their second birthday [2]. The HIV status of mothers and infants was well characterized through 1–2 years of follow-up, leading to the largest cohort to date of HEU infants (n = 3135), with a suitable comparison group of HIV-unexposed infants (n = 9510) This Review draws on 10 years of published data from this birth cohort, which has provided some of the strongest evidence to date of the poor health outcomes of HEU infants. The ZVITAMBO trial offered a unique opportunity to study HEU infants for several key reasons: first, maternal and infant HIV status was well characterized throughout follow-up (see below); second, the HIV-unexposed comparison group was similar and contemporaneous; third, the majority of infants in each group had similar feeding patterns (mixed breast-feeding); and, fourth, all infants had access to a free “sick clinic,” allowing similar assessment of morbidity status between groups

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