Institute of Biomedical Sciences, Academia Sinica, Taipei, Taiwan.
BMC Genet. 2005 Dec 30;6 Suppl 1(Suppl 1):S30. doi: 10.1186/1471-2156-6-S1-S30.
A thorough genetic mapping study was performed to identify predisposing genes for alcoholism dependence using the Collaborative Study on the Genetics of Alcoholism (COGA) data. The procedure comprised whole-genome linkage and confirmation analyses, single locus and haplotype fine mapping analyses, and gene x environment haplotype regression. Stratified analysis was considered to reduce the ethnic heterogeneity and simultaneously family-based and case-control study designs were applied to detect potential genetic signals. By using different methods and markers, we found high linkage signals at D1S225 (253.7 cM), D1S547 (279.2 cM), D2S1356 (64.6 cM), and D7S2846 (56.8 cM) with nonparametric linkage scores of 3.92, 4.10, 4.44, and 3.55, respectively. We also conducted haplotype and odds ratio analyses, where the response was the dichotomous status of alcohol dependence, explanatory variables were the inferred individual haplotypes and the three statistically significant covariates were age, gender, and max drink (the maximum number of drinks consumed in a 24-hr period). The final model identified important AD-related haplotypes within a candidate region of NRXN1 at 2p21 and a few others in the inter-gene regions. The relative magnitude of risks to the identified risky/protective haplotypes was elucidated.
采用协作性酒精中毒遗传学研究(COGA)的数据,进行了一项全面的遗传图谱研究,以鉴定导致酒精依赖的易感基因。该程序包括全基因组连锁和确认分析、单基因座和单体型精细定位分析,以及基因 x 环境单体型回归分析。分层分析被认为可以减少种族异质性,同时应用基于家庭和病例对照的研究设计来检测潜在的遗传信号。通过使用不同的方法和标记,我们在 D1S225(253.7 cM)、D1S547(279.2 cM)、D2S1356(64.6 cM)和 D7S2846(56.8 cM)处发现了高连锁信号,非参数连锁得分分别为 3.92、4.10、4.44 和 3.55。我们还进行了单体型和优势比分析,其中反应是酒精依赖的二分状态,解释变量是推断出的个体单体型,三个具有统计学意义的协变量是年龄、性别和最大饮酒量(24 小时内消耗的最大饮酒量)。最终模型确定了 NRXN1 位于 2p21 的候选区域内与 AD 相关的重要单体型,以及其他几个基因间区域的单体型。阐明了所确定的风险/保护单体型的相对风险程度。
