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19号染色体上与酒精依赖相关的连锁和关联证据。

Evidence for linkage and association to alcohol dependence on chromosome 19.

作者信息

Valdes A M, McWeeney S K, Thomson G

机构信息

Department of Integrative Biology, University of California, Berkeley 94720, USA.

出版信息

Genet Epidemiol. 1999;17 Suppl 1:S367-72. doi: 10.1002/gepi.1370170762.

Abstract

An association study on markers showing suggestive evidence for linkage to severe alcoholism was performed on the Collaborative Study on the Genetics of Alcoholism (COGA) data set. Our linkage study was restricted to the autosomal markers on chromosomes 2, 3, 4, 13, and 19, with low homozygosity (below 30%) and high identity-by-state sharing in affected sib pairs (ASPs). We used a strict phenotype definition, only individuals diagnosed as affected both on the ALDX1 (COGA criterion) and ALDX2 (ICD-10) scales were used in the analyses. Linkage was assessed by excess identity-by-descent allele sharing in ASPs. The strongest evidence of linkage was detected on chromosome 19, in particular at markers D19S49 (p < 0.0001) and D19S431 (p < 0.002). An association study of allele and haplotype data was then carried out on chromosome 19 markers using affected-family-based controls. A haplotype defined by alleles at markers D19S49, D19S43, and D19S200 in chromosome 19 shows significant association (p < 0.003, odds ratio 2.82). Further, significant differences were observed in the distribution of the harm avoidance subscale among genotypes defined by D19S49 (p < 0.0001). These results provide evidence for the existence of a locus in chromosome 19 potentially involved in alcohol dependence susceptibility.

摘要

在酒精中毒遗传学合作研究(COGA)数据集上,针对显示出与严重酒精中毒存在暗示性连锁证据的标记物进行了关联研究。我们的连锁研究仅限于2号、3号、4号、13号和19号染色体上的常染色体标记物,这些标记物在患病同胞对(ASP)中的纯合度较低(低于30%)且状态相同性共享度较高。我们使用了严格的表型定义,分析中仅纳入了在ALDX1(COGA标准)和ALDX2(国际疾病分类第10版)量表上均被诊断为患病的个体。通过患病同胞对中同源等位基因共享的过量情况来评估连锁。在19号染色体上检测到了最强的连锁证据,特别是在标记物D19S49(p < 0.0001)和D19S431(p < 0.002)处。然后,使用基于患病家庭的对照,对19号染色体标记物的等位基因和单倍型数据进行了关联研究。由19号染色体上标记物D19S49、D19S43和D19S200处的等位基因定义的单倍型显示出显著关联(p < 0.003,优势比2.82)。此外,在由D19S49定义的基因型中,回避伤害分量表的分布存在显著差异(p < 0.0001)。这些结果为19号染色体上可能参与酒精依赖易感性的一个基因座提供了存在证据。

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