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首页> 外文期刊>American Journal of Epidemiology >Maternal alcohol consumption, alcohol metabolism genes, and the risk of oral clefts: a population-based case-control study in Norway, 1996-2001.
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Maternal alcohol consumption, alcohol metabolism genes, and the risk of oral clefts: a population-based case-control study in Norway, 1996-2001.

机译:孕产妇饮酒,酒精代谢基因和口腔裂口的风险:挪威基于人群的病例对照研究,1996-2001年。

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Heavy maternal alcohol consumption during early pregnancy increases the risk of oral clefts, but little is known about how genetic variation in alcohol metabolism affects this association. Variants in the alcohol dehydrogenase 1C (ADH1C) gene may modify the association between alcohol and clefts. In a population-based case-control study carried out in Norway (1996-2001), the authors examined the association between maternal alcohol consumption and risk of oral clefts according to mother and infant ADH1C haplotypes encoding fast or slow alcohol-metabolizing phenotypes. Subjects were 483 infants with oral cleft malformations and 503 control infants and their mothers, randomly selected from all other livebirths taking place during the same period. Mothers who consumed 5 or more alcoholic drinks per sitting during the first trimester of pregnancy had an elevated risk of oral cleft in their offspring (odds ratio (OR) = 2.6, 95% confidence interval (CI): 1.4, 4.7). This increased risk was evident only in mothers or children who carried the ADH1C haplotype associated with reduced alcohol metabolism (OR= 3.0, 95% CI: 1.4, 6.8). There was no evidence of alcohol-related risk when both mother and infant carried only the rapid-metabolism ADH1C variant (OR = 0.9, 95% CI: 0.2, 4.1). The teratogenic effect of alcohol may depend on the genetic capacity of the mother and fetus to metabolize alcohol.
机译:孕早期孕妇大量饮酒会增加口腔裂伤的风险,但关于酒精代谢的遗传变异如何影响这种关联的知之甚少。酒精脱氢酶1C(ADH1C)基因的变体可能会改变酒精与left裂之间的关联。在挪威进行的一项基于人群的病例对照研究(1996-2001年)中,作者根据母婴ADH1C单倍型编码快速或慢速代谢酒精的表型,研究了母亲饮酒与口唇裂风险之间的关系。研究对象是从同一时期发生的所有其他活产中随机选择的483例口腔裂畸形婴儿和503例对照婴儿及其母亲。在怀孕的头三个月中,每次坐便喝5次或以上酒精饮料的母亲,其后代出现口腔裂的风险较高(优势比(OR)= 2.6,95%置信区间(CI):1.4、4.7)。仅在携带与酒精代谢降低相关的ADH1C单倍型的母亲或儿童中,这种风险增加才明显(OR = 3.0,95%CI:1.4,6.8)。当母亲和婴儿都仅携带快速代谢的ADH1C变异体时(OR = 0.9,95%CI:0.2,4.1),没有酒精相关风险的证据。酒精的致畸作用可能取决于母亲和胎儿代谢酒精的遗传能力。

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