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首页> 外文期刊>American journal of psychiatry >Association of the Alzheimer's gene SORL1 with hippocampal volume in young, healthy adults.
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Association of the Alzheimer's gene SORL1 with hippocampal volume in young, healthy adults.

机译:年轻健康的成年人中阿尔茨海默氏症基因SORL1与海马体积的关联。

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OBJECTIVE: Alzheimer's disease is among the most common neurodegenerative disorders. The SORL1 (sortilin receptor 1) gene is associated with the disease, but different variants seem to contribute. The authors used a gene-wide approach to test whether SORL1 is associated with volume of the hippocampus, one of the first structures to be affected by Alzheimer's disease in young, healthy individuals, in an attempt to map potential pathways from gene to disease. METHOD: Individuals were genotyped using an array-based method, and a total of 117 single nucleotide polymorphisms (SNPs) in and surrounding SORL1 were included in the analysis. Through the use of a brain segmentation protocol, SNP-by-SNP and gene-wide associations with bilateral hippocampal volume were assessed in two large, independent samples consisting of 446 (discovery cohort) and 490 (replication cohort) healthy young individuals. RESULTS: Significant association of the SORL1 gene with hippocampal volume was observed in both the discovery and replication samples as well as in the combined sample. The gene-wide association was independent of the apolipoprotein E genotype and resistant to removal of four significantly associated single SNPs. CONCLUSIONS: This study provides the first evidence that the SORL1 gene is associated with differences in hippocampal volume in young, healthy adults. It is demonstrated that gene-wide analysis techniques may overcome power problems caused by allelic heterogeneity in association studies. The results support the hypothesis that the SORL1 gene contributes to an increased risk for Alzheimer's disease through effects on hippocampal volume.
机译:目的:阿尔茨海默氏病是最常见的神经退行性疾病。 SORL1(sortilin受体1)基因与该疾病有关,但似乎有不同的变异。作者使用全基因范围的方法来测试SORL1是否与海马的体积有关,海马的体积是年轻健康个体中最早受阿尔茨海默氏病影响的结构之一,试图绘制从基因到疾病的潜在途径。方法:使用基于阵列的方法对个体进行基因分型,分析中共包含117个SORL1及其周围的单核苷酸多态性(SNP)。通过使用脑分割方案,在两个大的独立样本中评估了SNP-by-SNP和全基因范围与双侧海马体积的关联,这些样本由446个(发现队列)和490个(复制队列)健康的年轻个体组成。结果:发现和复制样品以及组合样品中均观察到SORL1基因与海马体积显着相关。全基因范围的关联独立于载脂蛋白E基因型,并且对去除四个显着相关的单个SNP具有抵抗力。结论:这项研究提供了第一个证据,表明SORL1基因与年轻健康成年人的海马体积差异有关。结果表明,全基因分析技术可以克服关联研究中等位基因异质性引起的能量问题。结果支持以下假设:SORL1基因通过影响海马体积而导致阿尔茨海默氏病风险增加。

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