首页> 美国卫生研究院文献>other >The Val66Met Brain-Derived Neurotrophic Factor Gene Variant Interacts with Early Pain Exposure to Predict Cortisol Dysregulation in 7-year-old Children Born Very Preterm: Implications for Cognition
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The Val66Met Brain-Derived Neurotrophic Factor Gene Variant Interacts with Early Pain Exposure to Predict Cortisol Dysregulation in 7-year-old Children Born Very Preterm: Implications for Cognition

机译:Val66Met脑源性神经营养因子基因变异与早期疼痛暴露相互作用以预测7岁出生的早产儿皮质醇调节异常:对认知的影响

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摘要

Early stress in the form of repetitive neonatal pain, in infants born very preterm, is associated with long-term dysregulation of the hypothalamic-pituitary-adrenal (HPA) axis and with poorer cognitive performance. Brain-derived neurotrophic factor (BDNF) which is important in synaptic plasticity and cognitive functions is reduced by stress. Therefore the BDNF Val66Met variant, which affects secretion of BDNF, may interact with early exposure to pain-related stress in children born very preterm, to differentially affect HPA regulation that in turn may be associated with altered cognitive performance.The aims of this study were to investigate whether in children born very preterm, the BDNF val66met variant modulates the association between neonatal pain-related stress and cortisol levels at age 7 years, and if cortisol levels were related to cognitive function. Furthermore, we examined whether these relationships were sex-specific. Using a longitudinal cohort design, N=90 children born very preterm (24–32 weeks gestation) were followed from birth to age 7 years. Cortisol was assayed from hair as an index of cumulative stress and from saliva to measure reactivity to a cognitive challenge. BDNF Val66Met variant was genotyped at 7 years using real time PCR. Using generalized linear modeling, in boys with the Met allele, greater neonatal pain-related stress (adjusted for clinical risk factors) predicted lower hair cortisol (p=0·006) and higher reactivity salivary cortisol (p=0.002). In both boys and girls with the Met allele, higher salivary cortisol reactivity was correlated with lower IQ (r= −0.60; p=0.001) and poorer visual-motor integration (r= −0.48; p=0.008).Our findings show associations between lower BDNF availability (presence of the Met allele) and vulnerability to neonatal pain/stress in boys, but not girls. This exploratory study suggests new directions for research into possible mechanisms underlying how neonatal pain/stress is related to cognitive performance in children born very preterm.
机译:对于早产儿,以反复性新生儿疼痛的形式出现的早期压力与下丘脑-垂体-肾上腺(HPA)轴的长期失调和认知能力较差有关。在突触可塑性和认知功能中起重要作用的脑源性神经营养因子(BDNF)会降低压力。因此,影响BDNF分泌的BDNF Val66Met变体可能与早产儿的早期暴露于疼痛相关的压力发生相互作用,从而差异性地影响HPA调节,进而可能与认知能力改变有关。为了研究是否在早产儿中,BDNF val66met变体是否调节了7岁时新生儿疼痛相关的压力与皮质醇水平之间的关联,以及皮质醇水平是否与认知功能有关。此外,我们检查了这些关系是否特定于性别。使用纵向队列设计,从出生到7岁的N = 90名早产儿(妊娠24-32周)进行了随访。从头发中测定皮质醇作为累积压力的指标,从唾液中测定皮质醇,以测量对认知挑战的反应性。使用实时PCR在7年时对BDNF Val66Met变体进行基因分型。使用广义线性模型,在具有Met等位基因的男孩中,较大的新生儿疼痛相关压力(针对临床危险因素进行了调整)可预测较低的头发皮质醇(p = 0·006)和较高的唾液皮质醇反应性(p = 0.002)。在具有Met等位基因的男孩和女孩中,唾液皮质醇反应性较高与智商较低(r = −0.60; p = 0.001)和视力整合较差(r = −0.48; p = 0.008)相关。较低的BDNF可用性(Met等位基因的存在)与男孩(而非女孩)对新生儿疼痛/应激的脆弱性之间的关系。这项探索性研究为研究早产儿新生儿疼痛/压力与认知能力之间的潜在机制提供了新的研究方向。

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