酒精性肝病遗传学研究进展

Ravi K Vishnubhotla, A. Kulkarni, Mithun Sharma, P. Rao, D. N. Reddy
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引用次数: 2

摘要

全世界估计有20亿人饮酒,这对健康和社会生活造成短期或长期后果。酒精每年造成约180万人死亡,占全球死亡总人数的3.2%。在20亿饮酒者中,超过7500万人被诊断为酒精使用障碍(AUD),并且患酒精性肝病(ALD)的风险增加。然而,并不是所有饮酒的人都会患上肝脏疾病,这表明宿主遗传与环境在表型沉淀中存在复杂的相互作用。随着基因组技术的进步,现在有可能对与表型相关的临床相关基因组位点进行精确测序,并且周转时间更快。变异形式的基因组数据可用于预测未受影响个体对表型的易感性,或可帮助临床医生预测疾病发病后的结果。这两者都至关重要,因为前者将有助于减轻疾病的未来负担,后者将有助于识别和治疗有严重肝病风险的个体。在当前的综述中,我们总结了ALD的致病机制,并讨论了迄今为止发现的可能有助于预测AUD患者酒精依赖和肝硬化发展的变异。
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An update on the genetics of alcoholic liver disease
Worldwide, an estimated 2 billion individuals consume alcohol, which contributes to short-term or long-term consequences on health and social life. Alcohol is the cause of approximately 1.8 million deaths per year, representing 3.2% of all deaths worldwide. Of the 2 billion individuals who consume alcohol, more than 75 million are diagnosed with alcohol-use disorder (AUD) and are at an enhanced risk of developing alcoholic liver disease (ALD). However, not all individuals who consume alcohol develop liver disease suggesting the intricate interactions of host genetics with the environment in the precipitation of the phenotype. With advances in genomic technologies, it is now possible to sequence clinically relevant genomic loci associated with a phenotype with precision and faster turnaround times. Genomic data in the form of variants may be used to predict susceptibility to a phenotype in an unaffected individual or may assist the clinician in predicting the outcomes after the onset of the disease. Both of these are crucial as the former would aid in reducing the future burden of the disease, and the latter would help identify and treat individuals at risk of severe liver disease. In the current review, we summarize the pathogenic mechanisms of ALD and discuss the variants identified to date that may aid in predicting alcohol dependence and the development of cirrhosis in individuals with AUD.
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