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Dissecting GI Phenotype – Genotype Relationships in GERD and Dyspepsia: An SNP Here and an SNP There!

机译:剖析GI表型– GERD和消化不良的基因型关系:这里有一个SNP那里有一个SNP!

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摘要

It is known that the predisposition to human disease is a mixture of inherited susceptibility and acquired exposure to environmental factors. Understanding gastrointestinal disease has indicated that germline adenomatous polyposis coli mutations predispose with a 99% certainty to colorectal cancer, whereas squamous esophageal cancer is caused by a combination of environmental exposures (including alcohol consumption, cigarette smoke, ingestion of contaminated preserved food) and/or infection (specifically with human papilloma virus), in most cases. Until now, despite the reasonably strong evidence for genetic risk from monozygotic twin studies for gastroesophageal reflux disease (GERD), there have been no documented genetic targets in GERD. In this edition of the Journal, there is intriguing evidence that a common, single base-pair change in the secondary messenger gene GNβ3 (i.e., a single-nucleotide polymorphism) may be important, perhaps through promoting abnormal perception of visceral pain in the esophagus. Other works link this genetic factor to functional dyspepsia, and these exciting preliminary lines of evidence are reviewed.
机译:众所周知,人类疾病的易感性是遗传易感性与获得的环境因素的混合。对胃肠道疾病的了解表明,生殖系腺瘤性息肉病大肠杆菌突变易使大肠癌发生99%的确定性,而食道鳞癌则是由环境暴露(包括饮酒,吸烟,摄入被污染的腌制食品)和/或多种因素共同引起的。在大多数情况下会感染(特别是人乳头瘤病毒)。到目前为止,尽管单卵双胎研究胃食管反流病(GERD)的遗传风险有相当有力的证据,但GERD中尚无记录的遗传靶标。在这一期的《华尔街日报》中,有趣的证据表明,次级信使基因GNβ3(即单核苷酸多态性)中常见的单个碱基对变化(可能是通过促进食道内脏痛的异常感知)可能很重要。 。其他工作将这种遗传因素与功能性消化不良联系起来,并对这些令人兴奋的初步证据进行了回顾。

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