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DRD2多巴胺受体基因型、连锁不平衡与美洲印第安人和其他人群的酗酒问题。

DRD2 dopamine receptor genotype, linkage disequilibrium, and alcoholism in American Indians and other populations.

作者信息

Goldman D, Brown G L, Albaugh B, Robin R, Goodson S, Trunzo M, Akhtar L, Lucas-Derse S, Long J, Linnoila M

机构信息

Laboratory of Neurogenetics, National Institute on Alcohol Abuse and Alcoholism, Bethesda, MD 20892.

出版信息

Alcohol Clin Exp Res. 1993 Apr;17(2):199-204. doi: 10.1111/j.1530-0277.1993.tb00749.x.

DOI:10.1111/j.1530-0277.1993.tb00749.x
PMID:8488955
Abstract

We defined interpopulation differences in the frequency of the dopamine D2 receptor DRD2/Taq1 A1 allele, which has previously been associated with alcoholism. Frequencies of the A1 allele in unrelated subjects were 0.18 to 0.20 (se = 0.02 to 0.03) in several Caucasian populations previously assessed, 0.38 (+/- 0.05) in American Blacks (n = 44), 0.63 (+/- 0.07) in Jemez Pueblo Indians (n = 23), and 0.80 (+/- 0.04) in Cheyenne Indians (n = 52). The existence of large interpopulation differences in the frequency of the Taq1 alleles suggests that associations to disease status could readily be generated or masked if disease and control groups were uneven in ethnic composition. To address the possibility that the 4-fold higher frequency of the A1 allele in Cheyenne Indians was related to an increased vulnerability to alcoholism in that population, 47 Cheyenne Indians were psychiatrically interviewed and blind-rated. However, there was no significant difference between interviewed controls (0.73 +/- 0.06, n = 24), subjects with alcoholism and/or drug abuse (0.74 +/- 0.06, n = 23) and noninterviewed population controls (0.87 +/- 0.05, n = 20). Legitimate association of the DRD2/Taq1 allele to alcoholism would presumably require it to be in linkage disequilibrium (nonrandom association) with a functional mutation at DRD2 or elsewhere. The level of disequilibrium would vary between populations and could place an upper bound on the strength of an association.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

我们定义了多巴胺D2受体DRD2/Taq1 A1等位基因频率的群体间差异,该等位基因此前已被认为与酗酒有关。在先前评估的几个白种人群体中,无关个体的A1等位基因频率为0.18至0.20(标准误=0.02至0.03),美国黑人中为0.38(±0.05)(n = 44),杰梅兹普韦布洛印第安人中为0.63(±0.07)(n = 23),夏延印第安人中为0.80(±0.04)(n = 52)。Taq1等位基因频率存在较大的群体间差异,这表明如果疾病组和对照组的种族构成不均衡,那么与疾病状态的关联很容易被产生或掩盖。为了探究夏延印第安人中A1等位基因频率高出4倍是否与该群体中酗酒易感性增加有关,我们对47名夏延印第安人进行了精神病学访谈并进行盲评。然而,接受访谈的对照组(0.73±0.06,n = 24)、患有酗酒和/或药物滥用的受试者(0.74±0.06,n = 23)与未接受访谈的群体对照组(0.87±0.05,n = 20)之间没有显著差异。DRD2/Taq1等位基因与酗酒的合理关联可能需要它与DRD2或其他位置的功能性突变处于连锁不平衡(非随机关联)状态。不平衡水平在不同群体间会有所不同,并且可能会对关联强度设置上限。(摘要截取自250字)

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