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首页> 外文期刊>World Journal of Gastroenterology >Liver enzymes, metabolomics and genome-wide association studies: From systems biology to the personalized medicine
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Liver enzymes, metabolomics and genome-wide association studies: From systems biology to the personalized medicine

机译:肝酶,代谢组学和全基因组关联研究:从系统生物学到个性化医学

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摘要

For several decades, serum levels of alanine (ALT) and aspartate (AST) aminotransferases have been regarded as markers of liver injury, including a wide range of etiologies from viral hepatitis to fatty liver. The increasing worldwide prevalence of metabolic syndrome and cardiovascular disease revealed that transaminases are strong predictors of type 2 diabetes, coronary heart disease, atherothrombotic risk profile, and overall risk of metabolic disease. Therefore, it is plausible to suggest that aminotransferases are surrogate biomarkers of “liver metabolic functioning” beyond the classical concept of liver cellular damage, as their enzymatic activity might actually reflect key aspects of the physiology and pathophysiology of the liver function. In this study, we summarize the background information and recent findings on the biological role of ALT and AST, and review the knowledge gained from the application of genome-wide approaches and “omics” technologies that uncovered new concepts on the role of aminotransferases in human diseases and systemic regulation of metabolic functions. Prediction of biomolecular interactions between the candidate genes recently discovered to be associated with plasma concentrations of liver enzymes showed interesting interconnectivity nodes, which suggest that regulation of aminotransferase activity is a complex and highly regulated trait. Finally, links between aminotransferase genes and metabolites are explored to understand the genetic contributions to the metabolic diversity.
机译:几十年来,血清丙氨酸(​​ALT)和天冬氨酸(AST)氨基转移酶水平一直被认为是肝损伤的标志物,包括从病毒性肝炎到脂肪肝的多种病因。全球范围内代谢综合征和心血管疾病的患病率上升表明,转氨酶是2型糖尿病,冠心病,动脉粥样硬化血栓形成风险谱以及代谢疾病总体风险的有力预测指标。因此,有可能表明氨基转移酶是“肝代谢功能”的替代生物标志物,超越了经典的肝细胞损伤概念,因为它们的酶活性可能实际上反映了肝功能生理学和病理生理学的关键方面。在这项研究中,我们总结了有关ALT和AST的生物学作用的背景信息和最新发现,并回顾了从全基因组方法和“组学”技术应用中获得的知识,这些技术揭示了关于氨基转移酶在人类中的作用的新概念疾病和代谢功能的全身调节。最近发现与肝酶血浆浓度相关的候选基因之间的生物分子相互作用的预测显示出有趣的互连性节点,这表明氨基转移酶活性的调节是一个复杂且高度受控的性状。最后,研究了氨基转移酶基因与代谢物之间的联系,以了解遗传对代谢多样性的贡献。

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