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胎盘下丘脑-垂体-肾上腺轴生物标志物的预测效用与婴儿神经发育

Predictive utility of placental hypothalamic-pituitary-adrenal axis biomarkers and infant neurodevelopment.

作者信息

Bakhireva Ludmila N, Ma Xingya, Wiesel Alexandria, Lowe Jean R, Rai Rajani, Solomon Elizabeth, Weinberg Joanne, Roberts Melissa H

机构信息

College of Pharmacy Substance Use Research and Education Center, University of New Mexico Health Sciences Center, Albuquerque, New Mexico, USA.

Department of Pediatrics, University of New Mexico, Health Sciences Center, Albuquerque, New Mexico, USA.

出版信息

J Neuroendocrinol. 2025 Jul 24:e70071. doi: 10.1111/jne.70071.

Abstract

Alcohol use remains common in pregnancy with prenatal alcohol exposure (PAE) associated with a plethora of adverse outcomes, including impaired emotional regulation and stress reactivity. Prior preclinical studies and emerging clinical evidence indicate that PAE affects the fetal hypothalamic-pituitary-adrenal (HPA) axis via the maternal-fetal interface in the placenta; however, little is known about the effect of these alterations on neurodevelopmental outcomes. We earlier reported on the effect of PAE and maternal stress on HPA axis biomarkers in placenta and umbilical cord (UC) blood; in the current study, we examined the effect of HPA axis biomarkers on infant neurodevelopmental outcomes at 6-9 months of term-equivalent age. Participants in the Ethanol, Neurodevelopment, Infant and Child Health (ENRICH-2) prospective cohort were followed from the second trimester of pregnancy until infants were 6-9 months of term-equivalent age. Maternal alcohol use was assessed through prospective interviews and a battery of ethanol biomarkers; maternal stress, by a Perceived Stress Scale (PSS). Placenta and UC blood specimens were collected shortly after birth, flash frozen, and analyzed for mRNA and protein expression of placental corticotropin-releasing hormone (pCRH), hydroxysteroid 11-beta dehydrogenase types 1 and 2 (HSD11B1, HSD11B2) and corresponding proteins (11β-HSD1 and 11β-HSD2), and Nuclear receptor subfamily 3 Group C Member 1-alpha (NR3C1-α) and corresponding glucocorticoid receptor alpha. UC plasma cortisol and cortisone levels were measured with ELISA. Bayley Scales of Infant Development, fourth edition (BSID-4; Motor, Language, Cognitive scores) and Infant Behavior Questionnaire Revised (IBQ-R; Surgency, Orienting/Regulation, Negative Affect) assessed neurodevelopment at 6-9 months of term-equivalent age. Pearson correlation was used to examine associations between placental HPA axis biomarkers and neurodevelopmental outcomes overall and after stratification by group (Alcohol/Control). Multivariable linear regression assessed the independent effect of placental biomarkers and Alcohol * biomarker interactions on infant outcomes after adjusting for Alcohol and maternal stress. Participants (32 Alcohol and 68 Controls) were comparable in sociodemographic characteristics. Activation of the placental HPA axis was correlated with a decrease in BSID-4 scores among Controls and an increase in IBQ-R scores (Surgency and Negative Affect) among Alcohol participants. In multivariable analyses, the HSD11B2/HSD11B1 ratio was associated with a decrease in Cognitive scores, and the Alcohol * pCRH interaction was associated with a decrease in Orienting/Regulation and an increase in Surgency and Negative Affect (all p's < .05), after adjusting for Alcohol and PSS. A significant independent effect of PSS was also observed on infant motor skills, Orienting/Regulation, and Negative Affect. This is the first clinical study to characterize the role of placental HPA axis biomarkers and maternal psychosocial stress in PAE-induced changes on infant neurodevelopment, highlighting the importance of a "placenta-brain axis". We demonstrated that the effects of mild-to-moderate PAE on infant neurobehavior were observed in participants with the highest quartile of pCRH expression, emphasizing the role of placental biomarkers in PAE-induced effects.

摘要

孕期饮酒仍然很常见,产前酒精暴露(PAE)与大量不良后果相关,包括情绪调节受损和应激反应性异常。先前的临床前研究和新出现的临床证据表明,PAE通过胎盘的母胎界面影响胎儿下丘脑 - 垂体 - 肾上腺(HPA)轴;然而,对于这些改变对神经发育结局的影响知之甚少。我们之前报道了PAE和母体应激对胎盘和脐带血中HPA轴生物标志物的影响;在本研究中,我们在足月等效年龄6 - 9个月时检查了HPA轴生物标志物对婴儿神经发育结局的影响。乙醇、神经发育、婴儿和儿童健康(ENRICH - 2)前瞻性队列研究的参与者从妊娠中期开始随访,直至婴儿达到足月等效年龄6 - 9个月。通过前瞻性访谈和一系列乙醇生物标志物评估母体饮酒情况;通过感知应激量表(PSS)评估母体应激。出生后不久收集胎盘和脐带血标本,速冻后分析胎盘促肾上腺皮质激素释放激素(pCRH)、1型和2型羟类固醇11 - β脱氢酶(HSD11B1、HSD11B2)及其相应蛋白(11β - HSD1和11β - HSD2)以及核受体亚家族3 C组成员1 - α(NR3C1 - α)及其相应糖皮质激素受体α的mRNA和蛋白表达。用酶联免疫吸附测定法(ELISA)测量脐带血血浆皮质醇和可的松水平。使用贝利婴儿发展量表第四版(BSID - 4;运动、语言、认知得分)和婴儿行为问卷修订版(IBQ - R;活力、定向/调节、消极情绪)在足月等效年龄6 - 9个月时评估神经发育情况。使用Pearson相关性分析来检查胎盘HPA轴生物标志物与总体神经发育结局之间以及按组(饮酒组/对照组)分层后的关联。多变量线性回归评估了在调整饮酒和母体应激因素后,胎盘生物标志物和饮酒生物标志物相互作用对婴儿结局的独立影响。参与者(32名饮酒组和68名对照组)在社会人口学特征方面具有可比性。胎盘HPA轴的激活与对照组中BSID - 4得分降低以及饮酒组参与者中IBQ - R得分(活力和消极情绪)升高相关。在多变量分析中,调整饮酒和PSS因素后,HSD11B2/HSD11B1比值与认知得分降低相关,饮酒pCRH相互作用与定向/调节降低以及活力和消极情绪升高相关(所有p值<0.05)。还观察到PSS对婴儿运动技能、定向/调节和消极情绪有显著的独立影响。这是第一项描述胎盘HPA轴生物标志物和母体心理社会应激在PAE诱导的婴儿神经发育变化中的作用的临床研究,突出了“胎盘 - 脑轴”的重要性。我们证明,在pCRH表达处于最高四分位数的参与者中观察到了轻度至中度PAE对婴儿神经行为的影响,强调了胎盘生物标志物在PAE诱导效应中的作用。

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