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An Integrated Multi-Omics Study Revealed Metabolic Alterations Underlying the Effects of Coffee Consumption

机译:一项综合的多组学研究揭示了咖啡消耗影响下的代谢变化

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Many epidemiological studies have indicated that coffee consumption may reduce the risks of developing obesity and diabetes, but the underlying mechanisms of these effects are poorly understood. Our previous study revealed the changes on gene expression profiles in the livers of C57BL/6J mice fed a high-fat diet containing three types of coffee (caffeinated, decaffeinated and green unroasted coffee), using DNA microarrays. The results revealed remarkable alterations in lipid metabolism-related molecules which may be involved in the anti-obesity effects of coffee. We conducted the present study to further elucidate the metabolic alterations underlying the effects of coffee consumption through comprehensive proteomic and metabolomic analyses. Proteomics revealed an up-regulation of isocitrate dehydrogenase (a key enzyme in the TCA cycle) and its related proteins, suggesting increased energy generation. The metabolomics showed an up-regulation of metabolites involved in the urea cycle, with which the transcriptome data were highly consistent, indicating accelerated energy expenditure. The TCA cycle and the urea cycle are likely be accelerated in a concerted manner, since they are directly connected by mutually providing each other's intermediates. The up-regulation of these pathways might result in a metabolic shift causing increased ATP turnover, which is related to the alterations of lipid metabolism. This mechanism may play an important part in the suppressive effects of coffee consumption on obesity, inflammation, and hepatosteatosis. This study newly revealed global metabolic alterations induced by coffee intake, providing significant insights into the association between coffee intake and the prevention of type 2 diabetes, utilizing the benefits of multi-omics analyses.
机译:许多流行病学研究表明,喝咖啡可以减少患肥胖症和糖尿病的风险,但是对这些影响的潜在机制了解甚少。我们以前的研究揭示了使用DNA微阵列喂养高脂饮食的C57BL / 6J小鼠肝脏中基因表达谱的变化,该饮食包含三种类型的咖啡(含咖啡因,无咖啡因和生绿色的咖啡)。结果表明,脂质代谢相关分子发生了显着变化,可能与咖啡的抗肥胖作用有关。我们进行了本研究,以通过全面的蛋白质组学和代谢组学分析进一步阐明咖啡摄入影响的代谢改变。蛋白质组学揭示了异柠檬酸脱氢酶(TCA循环中的关键酶)及其相关蛋白的上调,表明能量产生增加。代谢组学显示尿素循环中涉及的代谢物上调,其转录组数据高度一致,表明能量消耗加快。 TCA循环和尿素循环可能以协调的方式加速,因为它们通过相互提供彼此的中间体而直接连接。这些途径的上调可能导致代谢转变,从而导致ATP代谢增加,这与脂质代谢的改变有关。该机制可能在咖啡摄入对肥胖,炎症和肝脂肪变性的抑制作用中起重要作用。这项研究新发现了咖啡摄入引起的全球代谢变化,利用多组学分析的优势,为咖啡摄入与2型糖尿病的预防之间的关联提供了重要见解。

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