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产前暴露于有机磷酸酯代谢物与 MADRES 队列中早期运动发育的关系。

Prenatal exposures to organophosphate ester metabolites and early motor development in the MADRES cohort.

机构信息

Department of Population and Public Health Sciences, Keck School of Medicine, University of Southern California, Los Angeles, CA, USA.

Wadsworth Center, New York State Department of Health, Albany, NY, USA.

出版信息

Environ Pollut. 2024 Feb 1;342:123131. doi: 10.1016/j.envpol.2023.123131. Epub 2023 Dec 11.

Abstract

Organophosphate esters (OPEs) are increasingly considered neurotoxicants which may impact gross and fine motor development. We evaluated associations between prenatal OPE exposures and infant motor development. Third trimester urinary concentrations of nine OPE metabolites were measured in 329 mother-infant dyads participating in the Maternal And Developmental Risks from Environmental and Social Stressors (MADRES) cohort. Child gross and fine motor development at 6, 9, 12, and 18-months were assessed with the Ages and Stages Questionnaire-3 (ASQ-3) and operationalized in models using dichotomous instrument-specific cutoffs for typical motor development. Five OPE metabolites with >60% detection were specific-gravity-adjusted, natural log-transformed, and modeled continuously, while four metabolites with <60% detection were modeled dichotomously (detected/not-detected). We fit mixed effects logistic regression between OPE metabolites and fine/gross motor development and assessed sex-specific effects using a statistical interaction term and sex-stratified models. Among children, 31% and 23% had gross and fine motor scores, respectively, below the ASQ-3 at-risk cutoffs at least once across infancy. A doubling in prenatal diphenyl phosphate (DPHP) exposure was associated with 26% increased odds of potential fine motor delays (OR = 1.26, 95% CI: 1.02, 1.57, p = 0.04). We also observed significant interactions by infant sex for associations of detected dipropyl phosphate (DPRP) with gross motor development (p = 0.048) and detected bis(1-chloro-2-propyl) phosphate (BCIPP) with fine motor development (p = 0.02). Females had greater odds of potential motor delays for both detected DPRP (females vs males OR (95% CI) = 1.48 (0.71, 3.09), p = 0.30 vs 0.27 (0.06, 1.29), p = 0.10) and detected BCIPP (females vs males OR (95% CI) = 2.72 (1.27, 5.85), p = 0.01 vs 0.76 (0.31, 1.90), p = 0.56). There were no other significant associations between other metabolites and motor development, despite similar patterns. We found evidence of adverse effects of prenatal OPE exposures on infant motor development with greater adverse effects among female infants with some OPE metabolites.

摘要

有机磷酸酯 (OPE) 被认为是神经毒性物质,可能会影响大运动和精细运动的发展。我们评估了产前 OPE 暴露与婴儿运动发育之间的关联。在参与环境和社会应激源对母婴及发育风险研究(MADRES)队列的 329 对母婴中,测量了 329 对母婴的第三孕期尿液中 9 种 OPE 代谢物的浓度。使用年龄和阶段问卷-3(ASQ-3)评估了婴儿在 6、9、12 和 18 个月时的粗大和精细运动发育,并使用特定仪器的二分类截断值对典型运动发育进行模型化。对大于 60%检出率的 5 种 OPE 代谢物进行比重调整、自然对数转换并连续建模,而对小于 60%检出率的 4 种代谢物进行二分类建模(检出/未检出)。我们在 OPE 代谢物和精细/粗大运动发育之间拟合了混合效应逻辑回归,并使用统计学交互项和性别分层模型评估了性别特异性效应。在儿童中,分别有 31%和 23%的儿童在整个婴儿期至少有一次粗大运动和精细运动评分低于 ASQ-3 的风险截断值。产前二苯基磷酸酯 (DPHP) 暴露增加一倍,与潜在精细运动发育迟缓的几率增加 26%相关(OR=1.26,95%CI:1.02,1.57,p=0.04)。我们还观察到,在与粗大运动发育相关的检测到的二丙基磷酸酯 (DPRP)(p=0.048)和与精细运动发育相关的检测到的双(1-氯-2-丙基)磷酸酯 (BCIPP)(p=0.02)方面,婴儿性别存在显著的交互作用。对于两种检测到的 DPRP(女性 vs 男性 OR(95%CI)=1.48(0.71,3.09),p=0.30 vs 0.27(0.06,1.29),p=0.10)和检测到的 BCIPP(女性 vs 男性 OR(95%CI)=2.72(1.27,5.85),p=0.01 vs 0.76(0.31,1.90),p=0.56),女性发生潜在运动发育迟缓的几率更高。对于其他代谢物和运动发育之间没有其他显著的关联,尽管存在相似的模式。我们发现产前 OPE 暴露对婴儿运动发育有不良影响的证据,对于某些 OPE 代谢物,女婴的不良影响更大。

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