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首页> 外文期刊>Clinical and experimental allergy : >Genetic determinants of both ethanol and acetaldehyde metabolism influence alcohol hypersensitivity and drinking behaviour among Scandinavians.
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Genetic determinants of both ethanol and acetaldehyde metabolism influence alcohol hypersensitivity and drinking behaviour among Scandinavians.

机译:乙醇和乙醛代谢的遗传决定因素影响斯堪的纳维亚人的酒精超敏性和饮酒行为。

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BACKGROUND: Although hypersensitivity reactions following intake of alcoholic drinks are common in Caucasians, the underlying mechanisms and clinical significance are not known. In contrast, in Asians, alcohol-induced asthma and flushing have been shown to be because of a single nucleotide polymorphism (SNP), the acetaldehyde dehydrogenase 2 (ALDH2) 487lys, causing decreased acetaldehyde (the metabolite of ethanol) metabolism and high levels of histamine. However, the ALDH2 487lys is absent in Caucasians. OBJECTIVES: To investigate the genetic determinants of self-reported alcohol-induced hypersensitivity reactions in Caucasians. METHODS: The study included two population-based studies of 1216 and 6784 adults living in Copenhagen. Assessment of alcohol consumption and hypersensitivity reactions (in a subgroup) was performed by a questionnaire and was related to common SNPs of genes encoding alcohol dehydrogenases (ADHs) and ALDHs. RESULTS: In both populations, alcohol drinkers with a genetically determined fast metabolism of ethanol (the A allele of the ADH1b rs1229984) had an increased risk of alcohol-induced hypersensitivity reactions (odds ratio AA/AG vs. GG in combined populations: 1.82, 95% CI 1.04-3.17). In both populations, a common SNP encoding ALDH1b1 (rs2228093) was found to be significantly associated with alcohol-induced hypersensitivity (odds ratio TT vs. CC in combined populations: 2.53, 95% CI 1.31-4.90). CONCLUSIONS: Our data support that alcohol sensitivity in Caucasians is genetically determined and suggest that a histamine-releasing effect of acetaldehyde represents a plausible biological mechanism. Furthermore, we present the first report of a clinically significant SNP within the acetaldehyde-metabolizing system in a Caucasian population.
机译:背景:尽管高加索人在摄入酒精饮料后出现超敏反应,但其潜在机制和临床意义尚不清楚。相比之下,在亚洲人中,酒精引起的哮喘和潮红已被证明是由于单核苷酸多态性(SNP),乙醛脱氢酶2(ALDH2)487lys引起乙醛(乙醇的代谢产物)代谢下降和高水平的乙醛代谢所致。组胺。但是,高加索人没有ALDH2 487lys。目的:探讨白种人自我报告酒精引起的超敏反应的遗传决定因素。方法:该研究包括两项基于人口的居住在哥本哈根的1216和6784名成年人的研究。酒精消耗和超敏反应(在一个小组中)的评估是通过问卷进行的,并且与编码酒精脱氢酶(ADHs)和ALDHs的基因的常见SNP有关。结果:在这两个人群中,通过基因决定的乙醇快速代谢的酒精饮用者(ADH1b rs1229984的A等位基因)患酒精性超敏反应的风险增加(合并人群中的AA / AG与GG的比值比:1.82, 95%CI 1.04-3.17)。在这两个人群中,发现编码ALDH1b1的常见SNP(rs2228093)与酒精引起的超敏性显着相关(合并人群中TT与CC的比值比:2.53,95%CI 1.31-4.90)。结论:我们的数据支持高加索人对酒精的敏感性是由遗传决定的,并表明乙醛的组胺释放作用代表了可能的生物学机制。此外,我们提出了白人人群乙醛代谢系统中具有临床意义的SNP的首次报道。

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