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Using an Event-History with Risk-Free Model to Study the Genetics of Alcoholism

机译:使用事件历史和无风险模型研究酒精中毒的遗传学

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摘要

Case–control genetic association studies typically ignore possible later disease onset in currently healthy subjects and assume that subjects with diseases equally contribute to the likelihood for inference, regardless of their onset age. Therefore, we used an event-history with risk-free model to simultaneously characterize alcoholism susceptibility and onset age in 65 independent non-Hispanic Caucasian males in the Collaborative Study on the Genetics of Alcoholism. Following data quality control, we analysed 22 single nucleotide polymorphisms (SNPs) on 12 candidate genes. The single-SNP analysis showed that the dominant minor allele of rs2134655 on DRD3 increases alcoholism susceptibility; the dominant minor allele of rs1439047 on NTRK2 delays the alcoholism onset age, but the additive minor allele of rs172677 on GRIN2B and the dominant minor allele of rs63319 on ALDH1A1 advance the alcoholism onset age; and the dominant minor allele of rs1079597 on DRD2 shortens the onset age range. Similarly, multiple-SNPs analysis revealed joint effects of rs2134655, rs172677 and rs1079597, with an adjustment for habitual smoking. This study provides a more comprehensive understanding of the genetics of alcoholism than previous case–control studies.
机译:病例对照遗传关联研究通常会忽略当前健康受试者可能的较晚疾病发作,并假定患有疾病的受试者无论其发病年龄如何,均同样有助于推断。因此,在酒精中毒遗传学的合作研究中,我们使用无风险模型的事件历史记录来同时表征65名独立的非西班牙裔白人男性的酒精中毒易感性和发病年龄。根据数据质量控制,我们分析了12个候选基因上的22个单核苷酸多态性(SNP)。单单核苷酸多态性分析表明rs2134655在DRD3上的显性次要等位基因增加了酒精中毒的易感性。 NTRK2上rs1439047的显性次要等位基因延缓了酒精中毒的发病年龄,而GRIN2B上rs172677的加性次要等位基因和ALDH1A1上rs63319的显性次要等位基因延长了酒精中毒的发病年龄。而DRD2上rs1079597的显性次要等位基因则缩短了发病年龄范围。同样,多SNP分析显示rs2134655,rs172677和rs1079597的联合作用,并调整了习惯吸烟。这项研究比以前的病例对照研究提供了对酒精中毒遗传学的更全面的了解。

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