Alcohol drinking frequency is more directly associated with alcohol use disorder than alcohol metabolizing enzymes among male Japanese

Nishiyori, Atsushi; Shibata, Akira; Ogimoto, Itsuro; Uchimura, Naohisa; Egami, Hideki; Nakamura, Jun; Sakata, Ritsu; Fukuda, Katsuhiro

doi:10.1111/j.1440-1819.2005.01329.x

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Alcohol drinking frequency is more directly associated with alcohol use disorder than alcohol metabolizing enzymes among male Japanese
Citation	Nishiyori A, Shibata A, Ogimoto I, Uchimura N, Egami H, Nakamura J, Sakata R, Fukuda K. Psychiatry Clin. Neurosci. 2005; 59(1): 38-44.
Affiliation	Department of Public Health, Kurume University School of Medicine, Kurume, Japan. amiry@mte.biglobe.ne.jp
Copyright	(Copyright © 2005, John Wiley and Sons)
DOI	10.1111/j.1440-1819.2005.01329.x
PMID	15679538
Abstract	The development of alcohol use disorder (AUD) is related to various social, economic, cultural, environmental and hereditary factors. Several potential risk factors have been proposed for AUD in addition to alcohol consumption, including alcohol dehydrogenase2 (ADH2), acetaldehyde dehydrogenase2 (ALDH2), marital status, educational, occupational or past medical history (e.g. diabetes mellitus, hypertension, lung, digestive tract, or chronic liver disease) or smoking habits. The present study was performed to investigate the relationship between the aforementioned potential risk factors and AUD in Japan. A case-control study was performed on 153 male Japanese AUD patients and age-, gender-, or other confounder-matched controls to investigate the relation multivariately between ADH2, ALDH2 or alcohol drinking and AUD. Genomic DNA were extracted from nail clippings by the guanidium method, and genotyping of ADH2 and ALDH2 were performed using polymerase chain reaction-restriction fragment length polymorphism (PCR-RFLP) methods. Univariate analyses by the conditional logistic regression model revealed statistically significant odds ratios due to ADH21/1 genotype, ALDH21/1 genotype, middle school as the final school attended, longest occupations as farmers, fishermen, craftsmen, miners, production process or construction workers, and past histories of chronic liver disease and AUD. However, multivariate analyses under a hierarchically well-formulated model strategy with interaction and confounding assessment indicated that (i) heavy alcohol intake was a significant risk factor (odds ratio per 1.0 g of daily ethanol intake; 1.096, 95% confidence interval; 1.026-1.171) for developing AUD after adjusting for other confounders; and (ii) ADH21/1 genotype and ALDH21/1 genotype were not risk factors after adjusting for daily ethanol intake and other confounders. The present study shows that AUD was more directly and strongly associated with alcohol drinking than with alcohol metabolizing enzymes among male Japanese. Language: en