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早期生活环境、神经发育与特应性的关系。

Early life environment, neurodevelopment and the interrelation with atopy.

机构信息

Centre for Research in Environmental Epidemiology (CREAL), Barcelona, Spain.

出版信息

Environ Res. 2010 Oct;110(7):733-8. doi: 10.1016/j.envres.2010.07.005. Epub 2010 Aug 10.

Abstract

Both neurological and immunological systems are vulnerable to early life exposures. Neurological disorders and atopy have been related in animals and humans. Our main objective was to assess whether multiple exposures to early life determinants remain associated with neurodevelopment after considering the potential intermediate role of atopy. A second objective was to assess whether genes associated with atopy may inform about the potential neurotoxical mechanisms. Children were members of the AMICS birth cohort in Menorca (n=418, 87% of the recruited). General cognition was measured with the McCarthy Scales at age 4 and atopy through specific IgE at age 4 and prick test at age 6; 85 single nucleotide polymorphisms (SNPs) in 16 atopy and detoxification genes were genotyped. Among the 27 risk factors assessed, lower maternal social class, maternal smoking during pregnancy, being first born, shorter breastfeeding, higher DDT levels in cord blood, and higher indoor levels of NO2 (among the non-detoxifiers by GSTP1 polymorphism) were independently associated with poorer cognition. These associations were apparently not mediated by the relation between atopy and general cognition. Among the candidate atopic genes, variants in NQ01 (a detoxification gene) and NPRS1 (related with affective disorders like anxiety and stress management) had a significant association with general cognition (p-value<0.001). However, adjustment for the corresponding SNPs did not change the association between the early life determinants and general cognition. Multiple environmental pre-natal exposures were associated with neurodevelopment independently of their role in the immunological system. Atopic genes related to neurodevelopment suggest some potential mechanisms.

摘要

神经和免疫系统都容易受到生命早期暴露的影响。神经紊乱和过敏症在动物和人类中都有关联。我们的主要目的是评估早期生活决定因素的多重暴露在考虑过敏症的潜在中间作用后是否与神经发育相关。第二个目标是评估与过敏症相关的基因是否可以提供潜在的神经毒性机制的信息。儿童是梅诺卡岛 AMICS 出生队列的成员(n=418,占招募人数的 87%)。在 4 岁时使用 McCarthy 量表测量一般认知能力,在 4 岁时通过特异性 IgE 和 6 岁时的皮试测量过敏症;在 16 个过敏症和解毒基因中,85 个单核苷酸多态性(SNP)进行了基因分型。在评估的 27 个危险因素中,母亲的社会阶层较低、怀孕期间母亲吸烟、是第一个孩子、母乳喂养时间较短、脐带血中 DDT 水平较高、以及 GSTP1 多态性中室内 NO2 水平较高(非解毒剂)与认知能力较差独立相关。这些关联显然不是由过敏症与一般认知之间的关系介导的。在候选过敏症基因中,解毒基因 NQ01 和与焦虑和压力管理等情感障碍相关的 NPRS1 中的变异与一般认知有显著关联(p 值<0.001)。然而,对相应 SNP 的调整并未改变早期生活决定因素与一般认知之间的关联。多种产前环境暴露与神经发育有关,与它们在免疫系统中的作用无关。与神经发育相关的过敏症基因表明了一些潜在的机制。

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