Nicotine dependence in a prospective population-based study of adolescents: the protective role of a functional tyrosine hydroxylase polymorphism.

Richard J L Anney, Craig A Olsson, Mehrnoush Lotfi-Miri, George C Patton, Robert Williamson
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引用次数: 47

Abstract

Dopamine is a key neurotransmitter of the mesolimbic reward pathway in the human brain, and tyrosine hydroxylase (TH) is the rate-limiting enzyme in dopamine biosynthesis. Consequently, the gene encoding TH is a strong candidate for involvement in the genetic component of addiction. The importance of this gene in nicotine dependence is supported by many studies showing a link between nicotine administration and TH expression. A functional tetranucleotide repeat polymorphism within intron 1 of the TH gene (HUMTH01-VNTR) has been shown to modify tobacco use in two independent Caucasian samples from the USA and Australia. Using information drawn from an eight-wave Australian population-based longitudinal study of adolescent health, we tested the effect of the HUMTH01-VNTR on nicotine dependence. Comparisons were made between dependent smokers and non-dependent smokers. These data provide further support for a protective association between the K4 allele and dependent smoking (odds ratio 0.54, 95% confidence interval 0.28-1.0). No associations were observed at any of three other common TH polymorphisms (rs6356, rs6357 and HUMTH01-PstI). Including these data, three independent studies, two of which use identical phenotypes, have now identified a protective relationship between the K4 allele of the functional HUMTH01-VNTR polymorphism and high-level smoking.

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青少年尼古丁依赖的前瞻性人群研究:功能性酪氨酸羟化酶多态性的保护作用。
多巴胺是人脑中边缘奖赏通路的关键神经递质,酪氨酸羟化酶(tyrosine hydroxylase, TH)是多巴胺生物合成的限速酶。因此,编码TH的基因是参与成瘾遗传成分的强有力候选基因。该基因在尼古丁依赖中的重要性得到了许多研究的支持,这些研究表明尼古丁给药与TH表达之间存在联系。在来自美国和澳大利亚的两个独立的高加索人样本中,TH基因内含子1内的功能性四核苷酸重复多态性(HUMTH01-VNTR)已被证明可以改变烟草使用。利用来自澳大利亚八波青少年健康纵向研究的信息,我们测试了HUMTH01-VNTR对尼古丁依赖的影响。对依赖吸烟者和非依赖吸烟者进行了比较。这些数据进一步支持了K4等位基因与依赖吸烟之间的保护性关联(优势比0.54,95%可信区间0.28-1.0)。其他三种常见的TH多态性(rs6356、rs6357和HUMTH01-PstI)均未发现关联。包括这些数据,三个独立的研究,其中两个使用相同的表型,现在已经确定了功能性HUMTH01-VNTR多态性的K4等位基因与高水平吸烟之间的保护关系。
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