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从出生到幼儿期血浆全氟和多氟烷基物质(PFAS)水平的纵向轨迹、决定因素及代谢组学关联:波士顿出生队列的一项初步研究

Longitudinal trajectories and determinants of plasma per- and polyfluoroalkyl substance (PFAS) levels from birth to early childhood and metabolomic associations: A pilot study in the Boston Birth Cohort.

作者信息

Zhang Mingyu, Yu Chang Ho, Wang Guoying, Buckley Jessie P, Hong Xiumei, Pearson Colleen, Adams William G, Fan Zhihua Tina, Wang Xiaobin

机构信息

Department of Epidemiology, Johns Hopkins Bloomberg School of Public Health, Baltimore, MD, USA.

Welch Center for Prevention, Epidemiology, and Clinical Research, Johns Hopkins University, Baltimore, MD, USA.

出版信息

Precis Nutr. 2022 Jun;1(1). Epub 2022 Jun 13.

Abstract

BACKGROUND

Per- and polyfluoroalkyl substances (PFAS) are a major public health concern worldwide due to their ubiquitous exposures, environmental persistence, maternal-to-fetal transfer, and multi-organ toxicity. This pilot study aimed to generate preliminary data to inform future studies to address data gaps in the field, including early life PFAS exposure levels, longitudinal changes, determinants, and associated metabolomic alterations in understudied Black and Hispanic children in the United States (U.S.).

METHODS

This study leveraged existing biosamples and data in the Boston Birth Cohort and measured 12 legacy and emerging PFAS, including Me-PFOSA-AcOH, PFDA, PFDoA, PFHxS, PFNA, PFOA, PFOS, PFUnA, GenX, ADONA, 9Cl-PF3ONS, and PFHpS, in paired cord and early childhood plasma samples. Summary statistics and graphic plots were used to depict PFAS levels at the two time points and their longitudinal changes. Linear regression models were used to identify the early-life factors associated with cord and early childhood PFAS levels. Associations of cord PFAS with cord metabolites were explored using a metabolome-wide association approach and a targeted approach.

RESULTS

This study included 39 children, of whom 25 (64%) were Black, 14 (36%) were Hispanic, and 15 (38%) were female. PFOA, PFOS, PFNA, and PFHpS were detectable in all cord and early childhood plasma samples, while GenX and ADONA were not detectable in any sample. Cord PFAS levels were weakly-to-moderately correlated with early childhood PFAS levels ( = -0.03 to 0.40). Several maternal and child factors, including gestational age, year at blood collection, and race/ethnicity, were associated with cord and early childhood PFAS levels. The metabolome-wide association study and the targeted study identified several cord metabolites that may have been affected by PFAS exposure.

CONCLUSIONS

This pilot study found ubiquitous exposure to multiple PFAS in cord plasma (reflects exposure) and in early childhood plasma (reflects both prenatal and postnatal exposure) among U.S. Black and Hispanic children. Metabolomic analysis suggests that PFAS exposures may alter fetal metabolism. Future large-scale studies are needed to replicate the findings and further examine the associations of fetal PFAS exposure with long-term health outcomes and underlying metabolic pathways.

摘要

背景

全氟和多氟烷基物质(PFAS)因其广泛存在的暴露、环境持久性、母婴传递以及多器官毒性,成为全球主要的公共卫生问题。这项初步研究旨在生成初步数据,为未来研究提供信息,以填补该领域的数据空白,包括美国未被充分研究的黑人与西班牙裔儿童的早期生活中PFAS暴露水平、纵向变化、决定因素以及相关的代谢组学改变。

方法

本研究利用波士顿出生队列中现有的生物样本和数据,在配对的脐带血和幼儿血浆样本中测量了12种传统和新型PFAS,包括Me-PFOSA-AcOH、PFDA、PFDoA、PFHxS、PFNA、PFOA、PFOS、PFUnA、GenX、ADONA、9Cl-PF3ONS和PFHpS。使用汇总统计和图表来描述两个时间点的PFAS水平及其纵向变化。线性回归模型用于确定与脐带血和幼儿期PFAS水平相关的早期生活因素。使用全代谢组关联方法和靶向方法探索脐带血PFAS与脐带血代谢物之间的关联。

结果

本研究纳入了39名儿童,其中25名(64%)为黑人,14名(36%)为西班牙裔,15名(38%)为女性。在所有脐带血和幼儿血浆样本中均检测到PFOA、PFOS、PFNA和PFHpS,而在任何样本中均未检测到GenX和ADONA。脐带血PFAS水平与幼儿期PFAS水平呈弱至中度相关(相关系数=-0.03至0.40)。包括孕周、采血年份和种族/族裔在内的几个母婴因素与脐带血和幼儿期PFAS水平相关。全代谢组关联研究和靶向研究确定了几种可能受PFAS暴露影响的脐带血代谢物。

结论

这项初步研究发现,美国黑人与西班牙裔儿童的脐带血血浆(反映宫内暴露)和幼儿血浆(反映产前和产后暴露)中普遍存在多种PFAS暴露。代谢组学分析表明,PFAS暴露可能会改变胎儿代谢。未来需要进行大规模研究来重复这些发现,并进一步研究胎儿PFAS暴露与长期健康结果及潜在代谢途径之间的关联。

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