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HIV 阴性出生儿童的生长、身体和认知功能:津巴布韦农村一项集群随机试验的学龄期随访

Growth, physical, and cognitive function in children who are born HIV-free: School-age follow-up of a cluster-randomised trial in rural Zimbabwe.

机构信息

Zvitambo Institute for Maternal and Child Health Research, Harare, Zimbabwe.

Blizard Institute, Queen Mary University of London, London, United Kingdom.

出版信息

PLoS Med. 2024 Oct 11;21(10):e1004347. doi: 10.1371/journal.pmed.1004347. eCollection 2024 Oct.

Abstract

BACKGROUND

Globally, over 16 million children were exposed to HIV during pregnancy but remain HIV-free at birth and throughout childhood by 2022. Children born HIV-free (CBHF) have higher morbidity and mortality and poorer neurodevelopment in early life compared to children who are HIV-unexposed (CHU), but long-term outcomes remain uncertain. We characterised school-age growth, cognitive and physical function in CBHF and CHU previously enrolled in the Sanitation Hygiene Infant Nutrition Efficacy (SHINE) trial in rural Zimbabwe.

METHODS AND FINDINGS

The SHINE trial enrolled pregnant women between 2012 and 2015 across 2 rural Zimbabwean districts. Co-primary outcomes were height-for-age Z-score and haemoglobin at age 18 months (clinicaltrials.gov NCT01824940). Children were re-enrolled if they were aged 7 years, resident in Shurugwi district, and had known pregnancy HIV-exposure status. From 5,280 pregnant women originally enrolled, 376 CBHF and 2016 CHU reached the trial endpoint at 18 months in Shurugwi; of these, 264 CBHF and 990 CHU were evaluated at age 7 years using the School-Age Health, Activity, Resilience, Anthropometry and Neurocognitive (SAHARAN) toolbox. Cognitive function was evaluated using the Kaufman Assessment Battery for Children (KABC-II), with additional tools measuring executive function, literacy, numeracy, fine motor skills, and socioemotional function. Physical function was assessed using standing broad jump and handgrip for strength, and the shuttle-run test for cardiovascular fitness. Growth was assessed by anthropometry. Body composition was assessed by bioimpedance analysis and skinfold thicknesses. A caregiver questionnaire measured demographics, socioeconomic status, nurturing, child discipline, food, and water insecurity. We prespecified the primary comparisons and used generalised estimating equations with an exchangeable working correlation structure to account for clustering. Adjusted models used covariates from the trial (study arm, study nurse, exact child age, sex, calendar month measured, and ambient temperature). They also included covariates derived from directed acyclic graphs, with separate models adjusted for contemporary variables (socioeconomic status, household food insecurity, religion, social support, gender norms, caregiver depression, age, caregiver education, adversity score, and number of children's books) and early-life variables (length-for-age-Z-score) at 18 months, birthweight, maternal baseline depression, household diet, maternal schooling and haemoglobin, socioeconomic status, facility birth, and gender norms. We applied a Bonferroni correction for the 27 comparisons (0.05/27) with threshold of p < 0.00185 as significant. We found strong evidence that cognitive function was lower in CBHF compared to CHU across multiple domains. The KABC-II mental processing index was 45.2 (standard deviation (SD) 10.5) in CBHF and 48.3 (11.3) in CHU (mean difference 3.3 points [95% confidence interval (95% CI) 2.0, 4.5]; p < 0.001). The school achievement test score was 39.0 (SD 26.0) in CBHF and 45.7 (27.8) in CHU (mean difference 7.3 points [95% CI 3.6, 10.9]; p < 0.001); differences remained significant in adjusted analyses. Executive function was reduced but not significantly in adjusted analyses. We found no consistent evidence of differences in growth or physical function outcomes. The main limitation of our study was the restriction to one of two previous study districts, with possible survivor and selection bias.

CONCLUSIONS

In this study, we found that CBHF had reductions in cognitive function compared to CHU at 7 years of age across multiple domains. Further research is needed to define the biological and psychosocial mechanisms underlying these differences to inform future interventions that help CBHF thrive across the life-course.

TRIAL REGISTRATION

ClinicalTrials.gov The SHINE follow-up study was registered with the Pan-African Clinical Trials Registry (PACTR202201828512110). The original SHINE trial was registered at NCT https://clinicaltrials.gov/study/NCT01824940.

摘要

背景

在全球范围内,有超过 1600 万儿童在怀孕期间接触到了 HIV,但到 2022 年,仍有 1600 万儿童在出生时和整个儿童期保持 HIV 阴性。与未感染 HIV 的儿童(CHU)相比,出生时 HIV 阴性(CBHF)的儿童在生命早期的发病率和死亡率更高,且神经发育情况更差,但长期结果仍不确定。我们之前在津巴布韦农村地区的卫生与卫生习惯对婴儿营养功效(SHINE)试验中对以前入组的 CBHF 和 CHU 儿童进行了学校年龄生长、认知和身体功能的特征描述。

方法和发现

SHINE 试验在 2012 年至 2015 年期间在津巴布韦的 2 个农村地区招募了孕妇。主要结局指标是 18 个月时的身高年龄 Z 评分和血红蛋白(clinicaltrials.gov NCT01824940)。如果他们年满 7 岁,居住在舒鲁威区,且已知妊娠 HIV 暴露状况,则重新入组儿童。从最初招募的 5280 名孕妇中,有 376 名 CBHF 和 2016 名 CHU 在舒鲁威区达到了 18 个月的试验终点;其中,264 名 CBHF 和 990 名 CHU 在 7 岁时使用学校年龄健康、活动、适应力、人体测量和神经认知(SAHARAN)工具箱进行了评估。使用 Kaufman 儿童评估电池(KABC-II)评估认知功能,使用额外的工具测量执行功能、读写能力、计算能力、精细运动技能和社会情感功能。身体功能通过站立跳远和握力进行强度评估,通过穿梭跑测试进行心血管健康评估。生长通过人体测量法进行评估。身体成分通过生物阻抗分析和皮褶厚度进行评估。看护人调查问卷测量人口统计学、社会经济地位、养育、儿童纪律、食物和水不安全状况。我们预先指定了主要比较,并使用具有可交换工作相关结构的广义估计方程来解释聚类。调整后的模型使用来自试验的协变量(研究臂、研究护士、儿童确切年龄、性别、测量的日历月和环境温度)。它们还包括来自定向无环图的协变量,分别调整了当代变量(社会经济地位、家庭食物不安全、宗教、社会支持、性别规范、看护人抑郁、年龄、看护人教育、逆境评分和儿童书籍数量)和生命早期变量(年龄别身长 Z 评分),在 18 个月时、出生体重、母亲基线抑郁、家庭饮食、母亲教育和血红蛋白、社会经济地位、设施分娩和性别规范。我们对 27 项比较应用了 Bonferroni 校正(0.05/27),p<0.00185 作为显著阈值。我们发现了强有力的证据表明,在多个领域,CBHF 的认知功能低于 CHU。KABC-II 心理加工指数在 CBHF 中为 45.2(标准差(SD)10.5),在 CHU 中为 48.3(11.3)(平均差异 3.3 分[95%置信区间(95%CI)2.0,4.5];p<0.001)。学校成绩测试分数在 CBHF 中为 39.0(SD 26.0),在 CHU 中为 45.7(27.8)(平均差异 7.3 分[95%CI 3.6,10.9];p<0.001);在调整分析中差异仍然显著。执行功能虽然有所降低,但在调整分析中差异不显著。我们没有发现生长或身体功能结果存在差异的一致证据。我们研究的主要局限性是限制在以前研究的两个地区之一,可能存在幸存者和选择偏倚。

结论

在这项研究中,我们发现 CBHF 在 7 岁时的认知功能比 CHU 降低,涉及多个领域。需要进一步研究来确定这些差异背后的生物学和心理社会机制,以便为帮助 CBHF 在整个生命周期中茁壮成长的未来干预措施提供信息。

试验注册

PACTR202201828512110 是非洲临床试验注册中心(PACTR)对 SHINE 随访研究的注册信息。原始的 SHINE 试验在 clinicaltrials.gov 注册,注册号为 NCT01824940。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8f24/11498706/244fd6843188/pmed.1004347.g001.jpg

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