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Pooled association genome scanning: Validation and use to identify addiction vulnerability loci in two samples

机译:合并关联基因组扫描:验证并用于识别两个样本中的成瘾脆弱性基因座

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摘要

Association genome scanning is of increasing interest for identifying the chromosomal regions that contain gene variants that contribute to vulnerability to complex disorders, including addictions. To improve the power and feasibility of this approach, we have validated "10k" microarray-based allelic frequency assessments in pooled DNA samples and have used this approach to seek allelic frequency differences between heavy polysubstance abusers and well characterized control individuals. Thirty-eight loci contain SNPs that display robust allele frequency differences between abusers and controls in both European- and African-American samples. These loci identify an alcohol/acetaldehyde dehydrogenase gene cluster and genes implicated in cellular signaling, gene regulation, development, "cell adhesion," and Mendelian disorders. The results converge with previous linkage and association results for addictions. Pooled association genome-scanning provides a useful tool for elucidating molecular genetic underpinnings of complex disorders and identifies both previously understood and previously unanticipated mechanisms for addiction vulnerability.
机译:关联基因组扫描对于鉴定包含基因变异的染色体区域的兴趣日益增加,这些变异导致易患复杂疾病(包括成瘾)。为了提高此方法的功能和可行性,我们在合并的DNA样本中验证了基于“ 10k”基于微阵列的等位基因频率评估,并已使用该方法寻找重度多物质滥用者和特征明确的对照个体之间的等位基因频率差异。 38个基因座包含SNP,在欧洲和非裔美国人样本中,施虐者和对照之间均显示出强大的等位基因频率差异。这些基因座鉴定出醇/乙醛脱氢酶基因簇以及与细胞信号传导,基因调控,发育,“细胞粘附”和孟德尔疾病有关的基因。结果与成瘾的先前关联和关联结果一致。合并的关联基因组扫描为阐明复杂疾病的分子遗传基础提供了有用的工具,并可以识别成瘾易感性的先前了解和未曾预料的机制。

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