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Analysis of genetic polymorphisms of the dopaminergic and the serotonergic systems in drug dependent patients (Hungarian text).

机译:药物依赖患者多巴胺能和血清素能系统的遗传多态性分析(匈牙利语)。

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摘要

Substance dependence is a major social and health problem worldwide. It is generally accepted that genetic and environmental risk factors contribute to the development of drug addiction, however, at present, little is known about the exact nature and effects of its genetic components. The aim of the molecular genetic researches is to identify the genetic risk factors. One of the most widely used methods is the candidate gene association study.; Neurobiological models emphasize the key role of the reward system through the dopaminergic mesocorticolimbic pathway, which is modulated by a number of other neurotransmitters, such as serotonin. Genetic polymorphisms of several components of reward system (receptors, metabolizing enzymes, transporters) have been widely studied for association with various personality traits, as well as psychiatric disorders including substance dependence.; The present theses describe the elaboration [1] and the application [3,4] of a simplified, non invasive DNA sampling method; the genotyping of polymorphic regions including the coding region (DRD4 48 by VNTR) and the 5' upstream region (-521 C/T SNP [2]) and 120 by duplication) of the DRD4 gene; the investigation of the 5' upstream region (5HTTLPR), and the intron 2 polymorphism (STin2) of the SERT gene and the analysis of DRD4 and SERT gene polymorphisms as possible risk factors for substance dependence, in a case-control association study of 73 substance dependent subjects and 362 healthy Caucasian (Hungarian) controls [3,4].; Our results indicate significant association between the -521 C/T SNP of the DRD4 promoter region and heroin dependence (p = 0.044) and an interaction between the dopaminergic and serotonergic system at molecular level. Association between the -521 CC vs. CT or TT genotypes and heroin dependence was enhanced in the presence of 14-repeat 5HTTLPR allele (p 0.01). The observed odds ratio of 2.14 for the -521 CC genotype increased to 4.82 in case of the double homozygotes (i.e. -521 CC and 5HTTLPR 14/14), emphasizing the importance of combined analysis of polymorphisms in the dopaminergic and serotonergic systems in heroin dependence.
机译:物质依赖是世界范围内的主要社会和健康问题。人们普遍认为,遗传和环境危险因素会导致药物成瘾的发展,但是,目前,人们对其遗传成分的确切性质和作用知之甚少。分子遗传学研究的目的是确定遗传风险因素。候选基因关联研究是应用最广泛的方法之一。神经生物学模型通过多巴胺能的中皮层皮质寡糖途径强调奖励系统的关键作用,该途径受许多其他神经递质(如血清素)的调节。奖励系统的几个组成部分(受体,代谢酶,转运蛋白)的遗传多态性已被广泛研究,以与各种人格特征以及包括药物依赖在内的精神疾病相关。目前的论文描述了一种简化的,非侵入性的DNA采样方法的阐述[1]和应用[3,4]。 DRD4基因的编码区(VNTR的DRD4 48)和5'上游区(-521 C / T SNP [2]和120的重复)等多态区域的基因分型;在一项病例对照关联研究中,对SERT基因的5'上游区域(5HTTLPR)和内含子2多态性(STin2)进行了调查,并对DRD4和SERT基因多态性作为可能的物质依赖危险因素进行了分析依赖物质的受试者和362名健康的白种人(匈牙利)对照组[3,4]。我们的结果表明DRD4启动子区域的-521 C / T SNP与海洛因依赖性(p = 0.044)以及多巴胺能和血清素能系统在分子水平上的相互作用之间存在显着关联。在存在14个重复的5HTTLPR等位基因的情况下,-521 CC与CT或TT基因型与海洛因依赖之间的关联性得到增强(p <0.01)。在双重纯合子(即-521 CC和5HTTLPR 14/14)的情况下,-521 CC基因型的观察到的比值比为2.14,增加到4.82,强调了多巴胺能和血清素能系统多态性的联合分析对海洛因依赖性的重要性。

著录项

  • 作者

    Boor, Krisztina.;

  • 作者单位

    Semmelweis Egyetem (Hungary).;

  • 授予单位 Semmelweis Egyetem (Hungary).;
  • 学科 Biology Genetics.; Health Sciences Pharmacology.
  • 学位 Ph.D.
  • 年度 2005
  • 页码 94 p.
  • 总页数 94
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 遗传学;药理学;
  • 关键词

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