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首页> 外文期刊>Neuroscience Letters: An International Multidisciplinary Journal Devoted to the Rapid Publication of Basic Research in the Brain Sciences >DRD2/ANKK1 TaqIA and SLC6A3 VNTR polymorphisms in alcohol dependence: Association and gene-gene interaction study in a population of Central Italy
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DRD2/ANKK1 TaqIA and SLC6A3 VNTR polymorphisms in alcohol dependence: Association and gene-gene interaction study in a population of Central Italy

机译:DRD2 / ANKK1 TaqIA和SLC6A3 VNTR多态性与酒精依赖:在意大利中部人口的关联和基因-基因相互作用研究

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摘要

Dopamine is a neurotransmitter whose functions are mediated by five receptors expressed in several organs and tissues. Dopaminergic system dysfunctions are involved in the etiology or treatment of several pathological conditions, including drug addiction. Alcohol dependence (AD) is a widespread psychiatric disorder, affecting 5.4% of the general population lifetime. Family and twins studies support the role of a genetic component in AD. Since dopamine neurotransmission has been shown to be involved in drug reward, related genes are plausible candidates for susceptibility to AD. Here, we evaluated both the DRD2/ANKK1 TaqIA (rs1800497) and SLC6A3 40. bp-VNTR SNP and gene-gene interaction analysis in AD patients from a population of Central Italy. The study design was a case-control. In total, 280 alcoholic subjects (213 men and 67 woman) and 280 age- and sex-matched control subjects were recruited for this study. Case subjects met the DSM-IV criteria for AD and they are free from any psychiatric co-morbidities. Controls were subjects who had non-alcohol problem either never drank; those who have smoked at least one pack of cigarettes per day for at least 1 year were excluded. Genotyping was performed by allele-specific PCR and RFLP-PCR. SLC6A3 40. bp 3'UTR-VNTR displays no association with AD. DRD2/ANKK1 TaqIA genotype distribution is significantly associated to AD (O.R.= 1.551, p= 0.023), with A1 * allele displaying an O.R.= 1.403 (p= 0.029). Gene-gene interaction analysis using three-way contingency table analysis by a log-linear model yielded no significant result. Our study in a population of Central Italy extends and confirms previous results and, for the first time, tested the gene-gene interaction between SLC6A3 and DRD2 in AD.
机译:多巴胺是一种神经递质,其功能由几个器官和组织中表达的五个受体介导。多巴胺能系统功能异常涉及多种病理状况的病因或治疗,包括药物成瘾。酒精依赖(AD)是一种广泛的精神病,影响了整个人口寿命的5.4%。家庭和双胞胎研究支持遗传成分在AD中的作用。由于多巴胺神经传递已被证明参与药物奖励,因此相关基因是对AD易感性的合理候选者。在这里,我们评估了意大利中部人群AD患者的DRD2 / ANKK1 TaqIA(rs1800497)和SLC6A3 40. bp-VNTR SNP以及基因-基因相互作用分析。研究设计为病例对照。总共招募了280名酒精中毒受试者(213名男性和67名女性)以及280名年龄和性别相匹配的对照受试者。病例符合AD的DSM-IV标准,并且没有任何精神病合并症。对照组是没有饮酒问题的人,或者从未喝过酒。每天至少吸食一包香烟至少一年的人被排除在外。通过等位基因特异性PCR和RFLP-PCR进行基因分型。 SLC6A3 40. bp 3'UTR-VNTR与AD没有关联。 DRD2 / ANKK1 TaqIA基因型分布与AD显着相关(OR = 1.551,p = 0.023),而A1 *等位基因显示OR = 1.403(p = 0.029)。对数线性模型使用三向列联表分析法进行的基因-基因相互作用分析未得出明显结果。我们在意大利中部人口中的研究扩展并证实了先前的结果,并首次测试了AD中SLC6A3和DRD2之间的基因-基因相互作用。

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