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中西部阿米什人群中的帕金森病相关基因座。

Parkinson disease loci in the mid-western Amish.

机构信息

Center for Human Genetics Research, Vanderbilt University Medical Center, Nashville, TN, USA.

出版信息

Hum Genet. 2013 Nov;132(11):1213-21. doi: 10.1007/s00439-013-1316-1. Epub 2013 Jun 21.

Abstract

Previous evidence has shown that Parkinson disease (PD) has a heritable component, but only a small proportion of the total genetic contribution to PD has been identified. Genetic heterogeneity complicates the verification of proposed PD genes and the identification of new PD susceptibility genes. Our approach to overcome the problem of heterogeneity is to study a population isolate, the mid-western Amish communities of Indiana and Ohio. We performed genome-wide association and linkage analyses on 798 individuals (31 with PD), who are part of a 4,998 member pedigree. Through these analyses, we identified a region on chromosome 5q31.3 that shows evidence of association (p value < 1 × 10(-4)) and linkage (multipoint HLOD = 3.77). We also found further evidence of linkage on chromosomes 6 and 10 (multipoint HLOD 4.02 and 4.35 respectively). These data suggest that locus heterogeneity, even within the Amish, may be more extensive than previously appreciated.

摘要

先前的证据表明帕金森病(PD)具有遗传成分,但仅确定了 PD 总遗传贡献的一小部分。遗传异质性使拟议的 PD 基因的验证和新的 PD 易感性基因的鉴定变得复杂。我们克服异质性问题的方法是研究一个人群隔离群体,即印第安纳州和俄亥俄州中西部的阿米什社区。我们对 798 个人(31 人患有 PD)进行了全基因组关联和连锁分析,这些人是一个由 4998 名成员组成的家系的一部分。通过这些分析,我们确定了 5q31.3 染色体上的一个区域,该区域显示出关联的证据(p 值<1×10(-4))和连锁(多点 HLOD = 3.77)。我们还在 6 号和 10 号染色体上发现了进一步的连锁证据(多点 HLOD 分别为 4.02 和 4.35)。这些数据表明,即使在阿米什人中,位点异质性可能比以前认为的更为广泛。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4093/3797866/fd289ef5d72e/nihms497307f1.jpg

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