首页> 美国卫生研究院文献>other >GENETIC POLYMORPHISMS OF GRIN2A AND GRIN2B MODIFY THE NEUROBEHAVIORAL EFFECTS OF LOW-LEVEL LEAD EXPOSURE IN CHILDREN
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GENETIC POLYMORPHISMS OF GRIN2A AND GRIN2B MODIFY THE NEUROBEHAVIORAL EFFECTS OF LOW-LEVEL LEAD EXPOSURE IN CHILDREN

机译:GRIN2A和GRIN2B的遗传多态性改变儿童低水平铅暴露的神经行为影响

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摘要

Lead (Pb) is neurotoxic and children are highly susceptible to this effect, particularly within the context of continuous low-level Pb exposure. A current major challenge is identification of children who may be uniquely susceptible to Pb toxicity because of genetic predisposition. Learning and memory are among the neurobehavioral processes that are most notably affected by Pb exposure, and modification of N-methyl-D-aspartate receptors (NMDAR) that regulate these processes during development are postulated to underlie these adverse effects of Pb. We examined the hypothesis that polymorphic variants of genes encoding glutamate receptor, ionotropic, NMDAR subunits 2A and 2B, GRIN2A and GRIN2B, exacerbate the adverse effects of Pb exposure on these processes in children. Participants were subjects who participated as children in the Casa Pia Dental Amalgam Clinical Trial and for whom baseline blood Pb concentrations and annual neurobehavioral test results over the 7 year course of the clinical trial were available. Genotyping assays were performed for variants of GRIN2A (rs727605 and rs1070503) and GRIN2B (rs7301328 and rs1806201) on biological samples acquired from 330 of the original 507 trial participants. Regression modeling strategies were employed to evaluate the association between genotype status, Pb exposure, and neurobehavioral test outcomes. Numerous significant adverse interaction effects between variants of both GRIN2A and GRIN2B, individually and in combination, and Pb exposure were observed particularly among boys, preferentially within the domains of Learning & Memory and Executive Function. In contrast, very few interaction effects were observed among similarly genotyped girls with comparable Pb exposure. These findings support observations of an essential role of GRIN2A and GRIN2B on developmental processes underlying learning and memory as well as other neurological functions in children and demonstrate, further, modification of Pb effects on these processes by specific variants of both GRIN2A and GRIN2B genes. These observations highlight the importance of genetic factors in defining susceptibility to Pb neurotoxicity and may have important public health implications for future strategies aimed at protecting children and adolescents from potential health risks associated with low-level Pb exposure.
机译:铅(Pb)具有神经毒性,儿童特别是在连续低水平暴露于铅的情况下,高度易受这种影响。当前的主要挑战是鉴定由于遗传易感性而可能独特地对Pb毒性敏感的儿童。学习和记忆是受铅暴露最明显的神经行为过程之一,并且在发育过程中调节这些过程的N-甲基-D-天冬氨酸受体(NMDAR)的修饰被认为是铅的这些不利影响的基础。我们检查了一个假设,即编码谷氨酸受体,离子型,NMDAR亚基2A和2B,GRIN2A和GRIN2B的基因的多态性变体加剧了Pb暴露对儿童这些过程的不利影响。参加者是作为儿童参加“ Casa Pia牙科汞合金临床试验”的受试者,他们可获得临床试验7年中的基线血Pb浓度和年度神经行为测试结果。对从原始507名试验参与者中的330名获得的生物样品中进行了GRIN2A(rs727605和rs1070503)和GRIN2B(rs7301328和rs1806201)变异的基因分型测定。回归建模策略用于评估基因型状态,Pb暴露与神经行为测试结果之间的关联。 GRIN2A和GRIN2B的变体之间,无论是单独的还是组合的,都存在大量明显的不良相互作用,尤其是在男孩中,尤其是在学习与记忆和执行功能的范围内,Pb暴露也很明显。相比之下,在具有相似铅暴露水平的相似基因型女孩中,观察到很少的相互作用。这些发现支持了对GRIN2A和GRIN2B在儿童学习和记忆以及其他神经系统功能发育过程中必不可少的作用的观察,并进一步证明了GRIN2A和GRIN2B基因的特定变体修饰了Pb对这些过程的作用。这些发现强调了遗传因素在定义对铅神经毒性的敏感性中的重要性,并且可能对旨在保护儿童和青少年免受与低水平铅接触相关的潜在健康风险的未来策略具有重要的公共卫生影响。

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