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首页> 外文期刊>Genes, brain, and behavior >Genetic association analyses of PDYN polymorphisms with heroin and cocaine addiction.
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Genetic association analyses of PDYN polymorphisms with heroin and cocaine addiction.

机译:PDYN多态性与海洛因和可卡因成瘾的遗传关联分析。

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摘要

Genetic factors are believed to account for 30-50% of the risk for cocaine and heroin addiction. Dynorphin peptides, derived from the prodynorphin (PDYN) precursor, bind to opioid receptors, preferentially the kappa-opioid receptor, and may mediate the aversive effects of drugs of abuse. Dynorphin peptides produce place aversion in animals and produce dysphoria in humans. Cocaine and heroin have both been shown to increase expression of PDYN in brain regions relevant for drug reward and use. Polymorphisms in PDYN are therefore hypothesized to increase risk for addiction to drugs of abuse. In this study, 3 polymorphisms in PDYN (rs1022563, rs910080 and rs1997794) were genotyped in opioid-addicted [248 African Americans (AAs) and 1040 European Americans (EAs)], cocaine-addicted (1248 AAs and 336 EAs) and control individuals (674 AAs and 656 EAs). Sex-specific analyses were also performed as a previous study identified PDYN polymorphisms to be more significantly associated with female opioid addicts. We found rs1022563 to be significantly associated with opioid addiction in EAs [P = 0.03, odds ratio (OR) = 1.31; false discovery rate (FDR) corrected q-value]; however, when we performed female-specific association analyses, the OR increased from 1.31 to 1.51. Increased ORs were observed for rs910080 and rs199774 in female opioid addicts also in EAs. No statistically significant associations were observed with cocaine or opioid addiction in AAs. These data show that polymorphisms in PDYN are associated with opioid addiction in EAs and provide further evidence that these risk variants may be more relevant in females.
机译:据认为,遗传因素占可卡因和海洛因成瘾风险的30-50%。源自强啡肽(PDYN)前体的强啡肽与阿片受体结合,优先与κ阿片受体结合,并可能介导滥用药物的反作用。强啡肽在动物体内产生厌恶感,在人体内产生烦躁不安。可卡因和海洛因都已被证明可以增加与药物奖励和使用有关的大脑区域中PDYN的表达。因此,推测PDYN中的多态性会增加滥用药物成瘾的风险。在这项研究中,对PDYN(rs1022563,rs910080和rs1997794)的3个多态性进行了基因分型,分别是阿片类药物上瘾的[248名非洲裔美国人(AA)和1040名欧洲裔美国人(EAs)],可卡因上瘾的(1248 AAs和336 EA)和对照组(674个AA和656个EA)。由于先前的研究发现PDYN多态性与女性阿片类药物成瘾者更为显着相关,因此还进行了针对性别的分析。我们发现rs1022563与EA中的阿片类药物成瘾显着相关[P = 0.03,优势比(OR)= 1.31;错误发现率(FDR)校正的q值];但是,当我们进行女性特定的关联分析时,OR从1.31增加到1.51。在EA中,女性阿片类药物成瘾者中rs910080和rs199774的OR也增加。在AA中未观察到可卡因或阿片类药物成瘾的统计学显着关联。这些数据表明,PDYN中的多态性与EA中的阿片类药物成瘾有关,并提供了进一步的证据表明这些风险变异可能与女性更相关。

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