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Low frequency genetic variants in the mu-opioid receptor (OPRM1) affect risk for addiction to heroin and cocaine

机译:Mu-ApioID受体(OPRM1)中低频遗传变异影响对海洛因和可卡因成瘾的风险

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摘要

The μ-opioid receptor (MOR) binds exogenous and endogenous opioids and is known to mediate the rewarding effects of drugs of abuse. Numerous genetic studies have sought to identify common genetic variation in the gene encoding MOR (OPRM1) that affects risk for drug addiction. The purpose of this study was to examine the contribution of rare coding variants in OPRM1 to the risk for addiction. Rare and low frequency variants were selected using the National Heart Lung and Blood Institute –Exome Sequencing Project (NHLBI-ESP) database, which has screened the exomes of over 6500 individuals. Two SNPs (rs62638690 and rs17174794) were selected for genotyping in 1377 European American individuals addicted to heroin and/or cocaine. Two different SNPs (rs1799971 and rs17174801) were genotyped in 1238 African American individuals addicted to heroin and/or cocaine. Using the minor allele frequencies from the NHLBI-ESP dataset as a comparison group, case-control association analyses were performed. Results revealed an association between rs62638690 and cocaine and heroin addiction in European Americans (p=0.02; 95% C.I. 0.47 [0.24–0.92]). This study suggests a potential role for rare OPRM1 variants in addiction disorders and highlights an area worthy of future study.
机译:μ阿片受体(MOR)结合外源性和内源性阿片类药物,已知其介导滥用药物的有益作用。众多遗传学研究试图确定编码MOR(OPRM1)的基因中常见的遗传变异,这些变异会影响药物成瘾的风险。这项研究的目的是检查OPRM1中罕见的编码变异对成瘾风险的影响。使用美国国家心肺血液研究所外显子组测序项目(NHLBI-ESP)数据库选择了稀有和低频变异体,该数据库筛选了6500多个个体的外显子组。在1377年使海洛因和/或可卡因上瘾的欧美人中,选择了两个SNP(rs62638690和rs17174794)进行基因分型。在1238名对海洛因和/或可卡因上瘾的非洲裔美国人中对两种不同的SNP(rs1799971和rs17174801)进行了基因分型。使用来自NHLBI-ESP数据集的次要等位基因频率作为比较组,进行了病例对照关联分析。结果显示,rs62638690与可卡因和海洛因成瘾之间存在关联(p = 0.02; 95%C.I. 0.47 [0.24-0.92])。这项研究表明,罕见的OPRM1变异体在成瘾症中具有潜在的作用,并强调了一个值得进一步研究的领域。

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