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首页> 外文期刊>Biological psychiatry >Pro-opiomelanocortin gene variation related to alcohol or drug dependence: evidence and replications across family- and population-based studies.
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Pro-opiomelanocortin gene variation related to alcohol or drug dependence: evidence and replications across family- and population-based studies.

机译:与酒精或药物依赖性有关的促视神经黑皮质素基因变异:基于家庭和人群的研究的证据和重复。

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BACKGROUND: Opioidergic neurotransmission is critical in many, possibly all, forms of substance dependence. Several opioid-system genes have been shown to be associated with substance dependence disorders. The pro-opiomelanocortin gene (POMC) encodes several peptides important for endogenous opioidergic neurotransmission. We tested whether POMC genetic variation affects risk for substance dependence. METHODS: Five single nucleotide polymorphisms spanning POMC were examined in independent family and case-control samples. Family-based studies included 854 subjects from 319 African American (AA) families and 761 subjects from 313 European American (EA) families. Each family had a pair of siblings affected with cocaine and/or opioid dependence. Case-control studies included 791 cases (455 AAs and 336 EAs) affected with alcohol, cocaine, and/or opioid dependence and 682 control subjects (199 AAs and 483 EAs). RESULTS: Family-based analyses revealed an association of rs6719226 with opioid dependence in AA families and rs6713532 with cocaine dependence in EA families (p = .010-.044). Case-control analyses demonstrated an association of rs6713532 with alcohol or cocaine dependence in EAs (p(allele-wise) = .003-.008). Moreover, the minor allele of rs1866146 was found to be a risk factor for cocaine or opioid dependence in AAs (p(allele-wise) = .010-.017) and for alcohol, cocaine, or opioid dependence in EAs (p(allele-wise) = .001-.003). Logistic regression analyses in which sex and age were considered and population stratification analyses confirmed these findings. Additionally, specific haplotypes increased risk for cocaine dependence (p = .023) in AAs and opioid dependence (p = .012) in EAs. CONCLUSIONS: Given these replicated results, we conclude that variation in POMC confers vulnerability to multiple forms of substance dependence.
机译:背景:视力神经传递在许多形式的物质依赖中至关重要。已经显示几种阿片样物质系统基因与物质依赖性疾病有关。视紫红质皮质素原基因(POMC)编码几种对于内源性视皮醇能神经传递重要的肽。我们测试了POMC遗传变异是否影响物质依赖的风险。方法:在独立的家庭和病例对照样本中检查了跨越POMC的五个单核苷酸多态性。基于家庭的研究包括来自319个非洲裔美国人(AA)家庭的854个主题和来自313个非洲裔美国人(EA)的761个主题。每个家庭都有一对受可卡因和/或阿片类药物依赖影响的兄弟姐妹。病例对照研究包括791例(455个AA和336个EA)受酒精,可卡因和/或阿片类药物依赖,以及682个对照组(199个AA和483个EA)。结果:基于家庭的分析显示,AA家庭中rs6719226与阿片类药物依赖性相关,而EA家庭中与rs6713532与可卡因依赖性相关(p = .010-.044)。病例对照分析表明,在EA中rs6713532与酒精或可卡因依赖性相关(p(等位基因)= .003-.008)。此外,发现rs1866146的次要等位基因是AA中可卡因或阿片类药物依赖性的危险因素(p(等位基因)= .010-.017),而EAs中酒精,可卡因或阿片类药物依赖性(p(等位基因) -wise)= .001-.003)。考虑性别和年龄的逻辑回归分析以及人群分层分析证实了这些发现。此外,特定的单倍型会增加AA中可卡因依赖(p = .023)和EA中阿片类药物依赖(p = .012)的风险。结论:鉴于这些重复的结果,我们得出结论,POMC的变异赋予了对多种形式的物质依赖的脆弱性。

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