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Elevated Gestational IL-13 During Fetal Development Is Associated With Hyperactivity and Inattention in Eight-Year-Old Children

机译:胎儿发育过程中妊娠IL-13升高与八岁儿童的过度活跃和注意力不集中有关

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摘要

Maternal immune activation (MIA) during fetal development leads to behavioral and psychological disorders in the offspring. Concomitantly, insufficient supply of polyunsaturated fatty acids (PUFAs) is suspected to contribute to early neuronal maldevelopment due to the immune modulatory capabilities of PUFAs. However, human data are missing considering both of these aspects and their impact on children's behavioral outcomes. In line, this study aimed to elucidate the influence of gestational cytokines and PUFA-containing lipids during late pregnancy on behavioral sequelae in childhood, particularly focusing on an immune activation shaped by a history of maternal atopic diseases instead of a pathogen-mediated immune response. Based on the prospective mother-child cohort LINA we assessed the unstimulated blood cytokine profiles and concentrations of PUFA-containing lipids of 293 mothers at the 34th week of pregnancy. Maternal history of atopic diseases was obtained from questionnaires and behavior in eight-year-old children was assessed by the standardized Strength and Difficulties Questionnaires (SDQ) generating scores for hyperactivity/inattention, emotional symptoms, conduct problems, and peer relationship problems. Elevated IL-13 increased the risk for the child to show behavioral difficulties, in particular, hyperactive/inattentive behavior [adj. OR (95% CI): 2.47 (1.51–4.02), n = 255 vs. 38] at the age of eight years. Although the presence of maternal atopic dermatitis (AD) was associated with increased gestational IL-13 concentrations [adj. MR (95% CI): 1.17 (1.04–1.32)], no effect on children's behavioral difficulties was observed. However, a decrease in the PUFA containing lipid species PC aa C38:6 was not only associated with an increased gestational IL-13 concentration but also mediated the indirect effect of low PC aa C38:6 concentrations on children's abnormal behavior independent of maternal AD. We additionally assessed whether maternal IL-13 and PC aa C38:6 concentrations translate their effect by altering children's cord blood PC aa C38:6 and IL-13. While also the children's cord blood IL-13 was related to children's behavior, no effect of children's PC aa C38:6 was observed. This is the first study demonstrating that elevated gestational IL-13 increases the risk for children to develop behavioral difficulties. Analyses suggest that a reduced supply of gestational PC aa C38:6 contributes to elevated gestational IL-13 leading to behavioral sequelae in the offspring.
机译:胎儿发育过程中的母体免疫激活(MIA)会导致后代的行为和心理疾病。同时,由于PUFAs的免疫调节能力,怀疑多不饱和脂肪酸(PUFAs)供应不足会导致早期神经元发育不良。然而,考虑到这两个方面及其对儿童行为结果的影响,缺少了人类数据。与此一致,这项研究旨在阐明妊娠晚期妊娠细胞因子和含PUFA的脂质对儿童行为后遗症的影响,特别是关注由母源性特应性疾病史形成的免疫激活,而不是病原体介导的免疫反应。基于前瞻性母婴队列LINA,我们评估了怀孕第34周时未经刺激的血液细胞因子谱和293名母亲的含PUFA脂质的浓度。从问卷调查中获得母亲的特应性疾病病史,并通过标准化的“力量与困难问卷”(SDQ)评估了八岁儿童的行为,该问卷针对多动/注意力不集中,情绪症状,行为问题和同伴关系问题进行评分。 IL-13升高会增加儿童表现出行为障碍的风险,特别是活动过度/注意力不集中的行为[adj。或(95%CI):八岁时2.47(1.51-4.02),n = 255 vs. 38]。尽管母源性特应性皮炎(AD)的存在与妊娠IL-13浓度升高有关[adj。 MR(95%CI):1.17(1.04–1.32)],未观察到对儿童行为障碍的影响。但是,含PUFA的脂质物种PC aa C38:6的减少不仅与妊娠IL-13浓度升高有关,而且还介导了低PC aa C38:6浓度对儿童异常行为的间接影响,而与母体AD无关。我们还评估了母亲IL-13和PCaa C38:6的浓度是否通过改变儿童脐带血PCaa C38:6和IL-13的表达来转化其作用。尽管儿童的脐带血IL-13也与儿童的行为有关,但未观察到儿童PC氨基酸C38:6的影响。这是第一项研究,表明妊娠期IL-13升高会增加儿童发生行为障碍的风险。分析表明,妊娠PC aa C38:6的供应减少导致妊娠IL-13升高,导致后代的行为后遗症。

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