基于模式发现的方法分析μ-、δ-和κ-阿片受体基因变异对酒精或药物依赖的相互作用

Zhong Li, Huiping Zhang
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引用次数: 13

摘要

据报道,μ-、δ-和κ-阿片受体基因(OPRM1、OPRD1和OPRK1)的多态性与物质(酒精或药物)依赖有关。当在基因-基因相互作用的背景下分析时,个体基因对疾病性状的影响应该更加明显。因此,我们评估了这三种阿片受体基因变异对酒精、可卡因或阿片依赖的共同影响。方法从382例物质依赖的欧美人(其中酒精依赖318例,可卡因依赖171例,阿片依赖91例)和EA对照中获得13个OPRM1单核苷酸多态性(snp)、11个OPRD1 snp和7个OPRK1 snp的基因型数据。我们使用基于模式发现的关联测试评估了OPRM1、OPRD1和OPRK1变体对AD、CD或OD的联合影响。特定的标记模式(由OPRM1、OPRD1和OPRK1等位基因组成)在AD、CD或OD病例中比在对照组中明显更常见。结果在AD数据集中识别出12个显著模式,在CD数据集中识别出4个显著模式,在OD数据集中识别出18个显著模式。此外,大多数标记模式的重要性主要是由于OPRM1变异,在较小程度上是由于OPRD1变异。结论上述三种阿片受体基因的变异可能共同影响个体对酒精或药物依赖的易感性。本研究提供的证据也支持了之前的生物学发现,即三种阿片受体的相互作用可以调节阿片类药物和非阿片类药物以及酒精的作用。
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Analyzing Interaction of μ-, δ- and κ-opioid Receptor Gene Variants on Alcohol or Drug Dependence Using a Pattern Discovery-based Method
Background Polymorphisms in the μ-, δ- and κ-opioid receptor genes (OPRM1, OPRD1 and OPRK1) have been reported to be associated with substance (alcohol or drug) dependence. The influence of an individual gene on a disease trait should be more evident when analyzed in the context of gene-gene interactions. Thus, we assessed the joint effect of variants in these three opioid receptor genes on alcohol, cocaine, or opioid dependence. Methods Genotype data for 13 OPRM1 Single Nucleotide Polymorphisms (SNPs), 11 OPRD1 SNPs and seven OPRK1 SNPs were obtained from 382 European Americans (EAs) affected with substance dependence [among them, 318 with Alcohol Dependence (AD), 171 with Cocaine Dependence (CD), and 91 with Opioid Dependence (OD)] and 338 EA control subjects. We assessed the joint effect of OPRM1, OPRD1 and OPRK1 variants on AD, CD, or OD using a pattern discovery-based association test. Specific marker patterns (consisting of alleles of OPRM1, OPRD1 and OPRK1) that were significantly more frequent in AD, CD, or OD cases than in controls were identified. Results 12 significant patterns in the AD dataset, four significant patterns in the CD dataset, and 18 significant patterns in the OD dataset were identified. Moreover, the significance of most marker patterns was due primarily to OPRM1 variants and, to a lesser degree, OPRD1 variants. Conclusion Our findings suggest that variation in the above three opioid receptor genes can jointly influence the vulnerability of individuals to alcohol or drug dependence. Evidence provided by this study also supports previous biological findings that the interaction of the three opioid receptors can modulate the action of opioid and non-opioid drugs and alcohol.
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