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Gestational cytokine concentrations and neurocognitive development at 7 years

机译:7年妊娠细胞因子浓度和神经认知发育

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Gestational inflammation may contribute to brain abnormalities associated with childhood neuropsychiatric disorders. Limited knowledge exists regarding the associations of maternal cytokine levels during pregnancy with offspring neurocognitive development. We assayed the concentrations of five cytokines (interleukin (IL)-6, IL-1β, IL-8, tumor necrosis factor alpha (TNF-α), and IL-10) up to four times in the 2nd and 3rd trimesters of pregnancy using stored prenatal sera from 1366 participants in the New England Family Study (enrollment 1959–1966). Intelligence (IQ), academic achievement, and neuropsychological functioning of singleton offspring were assessed at age 7 years using standardized tests. We used linear mixed models with random effects to estimate the cumulative exposure to each cytokine during 2nd and 3rd trimesters, and then related cumulative cytokine exposure to a wide range of offspring neurocognitive outcomes. We found that children of women with higher levels of the pro-inflammatory cytokine, TNF-α, in the 2nd and 3rd trimesters had lower IQ ( B =??2.51, 99% CI: ?4.84,?0.18), higher problem scores in visual-motor maturity ( B =?0.12, 99% CI: 0.001,0.24), and lower Draw-a-Person test scores ( B =??1.28, 99% CI: ?2.49,?0.07). Higher gestational levels of IL-8, another pro-inflammatory molecule, were associated with better Draw-a-Person test scores and tactile finger recognition scores. Other cytokines were not associated with our outcome of interest. The opposing directions of associations observed between TNF-α and IL-8 with childhood outcomes suggest pleiotropic effects of gestational inflammation across the domains of neurocognitive functioning. Although the path to psychopathological disturbances in children is no doubt multifactorial, our findings point to a potential role for immune processes in the neurocognitive development of children.
机译:妊娠期炎症可能导致与儿童神经精神疾病有关的脑部异常。关于孕期母亲细胞因子水平与后代神经认知发育的关系,目前知之甚少。我们在妊娠的第三个和第三个三个月中测定了多达四次的五种细胞因子(白介素(IL)-6,IL-1β,IL-8,肿瘤坏死因子α(TNF-α)和IL-10)的浓度使用新英格兰家庭研究(1959–1966年招生)中1366名参与者的存储的产前血清。在7岁时使用标准化测试评估了单胎后代的智力(IQ),学习成绩和神经心理学功能。我们使用具有随机效应的线性混合模型来估计第2和第3孕期每种细胞因子的累积暴露,然后将累积细胞因子的暴露与广泛的后代神经认知结果相关。我们发现,在第2和第3个孕期中促炎性细胞因子TNF-α含量较高的女性儿童的智商较低(B = ?? 2.51,99%CI:?4.84,?0.18),问题得分更高视觉运动成熟度(B =?0.12,99%CI:0.001,0.24)和较低的Draw-a-Person测试得分(B =?1.28,99%CI:?2.49,?0.07)。较高的妊娠水平IL-8(另一个促炎分子)与较好的Draw-a-Person测试成绩和触觉手指识别成绩相关。其他细胞因子与我们感兴趣的结果无关。 TNF-α和IL-8与儿童期结局之间的相反关联方向表明,在神经认知功能的整个领域中,妊娠炎症的多效性作用。尽管毫无疑问,儿童心理病理障碍的途径是多因素的,但我们的发现指出了免疫过程在儿童神经认知发育中的潜在作用。

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