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Histone modifications and alcohol-induced liver disease: Are altered nutrients the missing link?

机译:组蛋白修饰和酒精引起的肝病:营养成分改变是否缺失?

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摘要

Alcoholism is a major health problem in the United States and worldwide, and alcohol remains the single most significant cause of liver-related diseases and deaths. Alcohol is known to influence nutritional status at many levels including nutrient intake, absorption, utilization, and excretion, and can lead to many nutritional disturbances and deficiencies. Nutrients can dramatically affect gene expression and alcohol-induced nutrient imbalance may be a major contributor to pathogenic gene expression in alcohol-induced liver disease (ALD). There is growing interest regarding epigenetic changes, including histone modifications that regulate gene expression during disease pathogenesis. Notably, modifications of core histones in the nucleosome regulate chromatin structure and DNA methylation, and control gene transcription. This review highlights the role of nutrient disturbances brought about during alcohol metabolism and their impact on epigenetic histone modifications that may contribute to ALD. The review is focused on four critical metabolites, namely, acetate, S-adenosylmethionine, nicotinamide adenine dinucleotide and zinc that are particularly relevant to alcohol metabolism and ALD.
机译:酒精中毒是美国和世界范围内的主要健康问题,酒精仍然是与肝脏有关的疾病和死亡的唯一最重要的原因。众所周知,酒精会在许多水平上影响营养状况,包括营养摄入,吸收,利用和排泄,并可能导致许多营养紊乱和营养缺乏。营养物质可显着影响基因表达,酒精诱导的营养失衡可能是酒精诱导的肝病(ALD)中致病基因表达的主要贡献者。对于表观遗传学的改变,包括在疾病发病过程中调节基因表达的组蛋白修饰,人们越来越感兴趣。值得注意的是,核小体中核心组蛋白的修饰可调节染色质结构和DNA甲基化,并控制基因转录。这篇综述强调了酒精代谢过程中营养紊乱的作用,以及它们对可能导致ALD的表观遗传组蛋白修饰的影响。综述集中在与乙醇代谢和ALD特别相关的四种关键代谢物,即乙酸盐,S-腺苷甲硫氨酸,烟酰胺腺嘌呤二核苷酸和锌。

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