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健康受试者与酗酒者血浆多巴胺β-羟化酶的基因型对照分析:去甲肾上腺素能功能存在与酒精相关差异的证据

A genotype-controlled analysis of plasma dopamine beta-hydroxylase in healthy and alcoholic subjects: evidence for alcohol-related differences in noradrenergic function.

作者信息

Köhnke Michael D, Zabetian Cyrus P, Anderson George M, Kolb Werner, Gaertner Ines, Buchkremer Gerhard, Vonthein Reinhard, Schick Sandra, Lutz Ulrich, Köhnke Annette M, Cubells Joseph F

机构信息

University Hospital of Psychiatry and Psychotherapy, Tübingen University Hospital, Tübingen, Germany.

出版信息

Biol Psychiatry. 2002 Dec 15;52(12):1151-8. doi: 10.1016/s0006-3223(02)01427-0.

DOI:10.1016/s0006-3223(02)01427-0
PMID:12488060
Abstract

BACKGROUND

Norepinephrine and dopamine mediate important aspects of alcoholism and alcohol withdrawal. Dopamine-beta-hydroxylase (DbetaH) converts dopamine to norepinephrine. A recent study demonstrated a strong association between variance in plasma DbetaH activity and a novel polymorphism (DBH-1021C-->T) at the structural locus (DBH) encoding DbetaH protein.

METHODS

Our study investigated whether the DBH-1021C-->T polymorphism and plasma DbetaH activity were associated with alcoholism or with delirium tremens (DT) during alcohol withdrawal by analyzing 207 German alcoholic and 102 healthy control subjects. We also examined the influence of the polymorphism on enzyme activity.

RESULTS

Mean (+SD) plasma DbetaH activity measured in alcoholic subjects abstinent was significantly lower than that observed in control (27.7 + 16.7 vs. 35.6 + 18.8; p =.01). It did not differ between subjects with DT during withdrawal and subjects with mild withdrawal symptoms. The T allele of the DBH-1021C-->T polymorphism was significantly associated with lower plasma DbetaH activity. None of the alleles or genotypes were associated with alcoholism or DT.

CONCLUSIONS

The data indicate that the alcoholism-related reduction in plasma DbetaH activity is independent of genotype at DBH-1021C-->T and replicate the finding that DBH-1021C-->T is strongly associated with plasma DbetaH activity in a native Western European population.

摘要

背景

去甲肾上腺素和多巴胺在酒精中毒及酒精戒断过程中发挥着重要作用。多巴胺-β-羟化酶(DβH)可将多巴胺转化为去甲肾上腺素。最近一项研究表明,血浆DβH活性的变化与编码DβH蛋白的结构基因座(DBH)处的一种新型多态性(DBH-1021C→T)之间存在密切关联。

方法

我们的研究通过分析207名德国酗酒者和102名健康对照者,调查了DBH-1021C→T多态性及血浆DβH活性是否与酒精中毒或酒精戒断期间的震颤谵妄(DT)相关。我们还研究了该多态性对酶活性的影响。

结果

戒酒的酗酒者的平均(+标准差)血浆DβH活性显著低于对照组(27.7 + 16.7对35.6 + 18.8;p = 0.01)。在戒断期间出现DT的患者与有轻度戒断症状的患者之间,该活性并无差异。DBH-1021C→T多态性的T等位基因与较低的血浆DβH活性显著相关。没有任何等位基因或基因型与酒精中毒或DT相关。

结论

数据表明,与酒精中毒相关的血浆DβH活性降低与DBH-1021C→T的基因型无关,并再次证实了在西欧本土人群中DBH-1021C→T与血浆DβH活性密切相关这一发现。

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