Across-Site Differences in the Mechanism of Alcohol-Induced Digestive Tract Carcinogenesis: An Evaluation by Mediation Analysis

ALDH2 癌症 胃肠道 内科学 医学 癌变 胃肠病学 乙醛 醛脱氢酶 头颈部癌 结直肠癌 致癌物 胃癌 食管癌 肿瘤科 生物 乙醇 遗传学 生物化学 基因
作者
Yuriko N. Koyanagi,Etsuji Suzuki,Issei Imoto,Yumiko Kasugai,Isao Oze,Tomotaka Ugai,Madoka Iwase,Yoshiaki Usui,Yukino Kawakatsu,Michi Sawabe,Yutaka Hirayama,Tsutomu Tanaka,Tetsuya Abe,Seiji Ito,Koji Komori,Nobuhiro Hanai,Masahiro Tajika,Yasuhiro Shimizu,Yasumasa Niwa,Hidemi Ito,Keitaro Matsuo
出处
期刊:Cancer Research [American Association for Cancer Research]
卷期号:80 (7): 1601-1610 被引量:23
标识
DOI:10.1158/0008-5472.can-19-2685
摘要

Abstract A genetic variant on aldehyde dehydrogenase 2 (ALDH2 rs671, Glu504Lys) contributes to carcinogenesis after alcohol consumption. Somewhat conversely, the ALDH2 Lys allele also confers a protective effect against alcohol-induced carcinogenesis by decreasing alcohol consumption due to acetaldehyde-related adverse effects. Here, we applied a mediation analysis to five case–control studies for head and neck, esophageal, stomach, small intestine, and colorectal cancers, with 4,099 cases and 6,065 controls, and explored the potentially heterogeneous impact of alcohol drinking on digestive tract carcinogenesis by decomposing the total effect of the ALDH2 Lys allele on digestive tract cancer risk into the two opposing effects of the carcinogenic effect (direct effect) and the protective effect (indirect effect mediated by drinking behavior). Alcohol was associated with an increased risk of most digestive tract cancers, but significant direct effects were observed only for upper gastrointestinal tract cancer risk, and varied substantially by site, with ORs (95% confidence interval) of 1.83 (1.43–2.36) for head and neck cancer, 21.15 (9.11–49.12) for esophageal cancer, and 1.65 (1.38–1.96) for stomach cancer. In contrast, a significant protective indirect effect was observed on risk for all cancers, except small intestine cancer. These findings suggest that alcohol is a major risk factor for digestive tract cancers, but its impact as a surrogate for acetaldehyde exposure appears heterogeneous by site. Meanwhile, the behavior-related effect of the ALDH2 Lys allele results in a decreased risk of most digestive tract cancers. Significance: These findings support that genetic alcohol avoidance is a factor against alcohol-induced cancers.

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