In Utero Antiretroviral Exposure and Risk of Neurodevelopmental Problems in HIV-Exposed Uninfected 5-Year-Old Children

医学 阿扎那韦 优势比 洛比那韦 养生 置信区间 混淆 人口 儿科 恩曲他滨 齐多夫定 怀孕 队列研究 内科学 病毒载量 免疫学 人类免疫缺陷病毒(HIV) 环境卫生 抗逆转录病毒疗法 病毒性疾病 生物 遗传学
作者
Tzy‐Jyun Yao,Kathleen Malee,Joel Zhang,Renee Smith,Sean M. Redmond,Mabel L. Rice,Toni Frederick,Peter Torre,Claude A. Mellins,Howard J. Hoffman,Paige L. Williams
出处
期刊:Aids Patient Care and Stds [Mary Ann Liebert, Inc.]
卷期号:37 (3): 119-130 被引量:5
标识
DOI:10.1089/apc.2022.0189
摘要

Studies have observed neurodevelopmental (ND) challenges among young children perinatally HIV-exposed yet uninfected (CHEU) with in utero antiretroviral (ARV) exposure, without clear linkage to specific ARVs. Atazanavir (ATV) boosted with ritonavir has been a preferred protease inhibitor recommended for pregnant women, yet associations of ATV with ND problems in CHEU have been reported. Studies among early school-age children are lacking. The pediatric HIV/AIDS cohort study (PHACS) surveillance monitoring for antiretroviral therapy (ART) toxicities (SMARTT) study evaluated 5-year-old monolingual English-speaking CHEU using the behavior assessment system for children, Wechsler preschool and primary scales of intelligence, and test of language development-primary. A score ≥1.5 standard deviations worse than population norms defined a signal within each domain. Analyses of risk for signals were stratified by timing of any ARV initiation. Associations between ARV exposure and risk of ND signals were assessed using proportional odds models, adjusting for confounders. Among 230 children exposed to ARVs at conception, 15% had single and 8% had multiple ND problems; ATV exposure was not associated with higher risk of signals [adjusted cumulative odds ratio (cOR) = 0.66, confidence interval (CI): 0.28–1.56]. However, among 461 children whose mothers initiated ARVs during pregnancy, 21% had single and 12% had multiple ND problems; ATV exposure was associated with higher risk of signals (cOR = 1.70, CI: 0.82–3.54). The specific regimen tenofovir/emtricitabine/ATV was associated with higher risk (cOR = 2.31, CI: 1.08–4.97) relative to regimens using a zidovudine/lamivudine backbone combined with non-ATV ARVs. It remains important to monitor neurodevelopment of CHEU during early childhood and investigate the impact and the role of timing of in utero exposure to specific ARVs.
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