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首页> 外文期刊>Frontiers in Pharmacology >Aqueous Extract of Black Maca Prevents Metabolism Disorder via Regulating the Glycolysis/Gluconeogenesis-TCA Cycle and PPARα Signaling Activation in Golden Hamsters Fed a High-Fat, High-Fructose Diet
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Aqueous Extract of Black Maca Prevents Metabolism Disorder via Regulating the Glycolysis/Gluconeogenesis-TCA Cycle and PPARα Signaling Activation in Golden Hamsters Fed a High-Fat, High-Fructose Diet

机译:黑玛卡水提取物可通过调节高脂,高果糖饮食的金黄仓鼠中的糖酵解/糖异生-TCA循环和PPARα信号激活来预防代谢紊乱

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Maca ( Lepidium meyenii Walpers) has been used as a dietary supplement and ethnomedicine for centuries. Recently, maca has become a high profile functional food worldwide because of its multiple biological activities. This study is the first explorative research to investigate the prevention and amelioration capacity of the aqueous extract of black maca (AEM) on high-fat, high-fructose diet (HFD)-induced metabolism disorder in golden hamsters and to identify the potential mechanisms involved in these effects. For 20 weeks, 6-week-old male golden hamsters were fed the following respective diets: (1) a standard diet, (2) HFD, (3) HFD supplemented with metformin, or (4) HFD supplemented with three doses of AEM (300, 600, or 1,200 mg/kg). After 20 weeks, the golden hamsters that received daily AEM supplementation presented with the beneficial effects of improved hyperlipidemia, hyperinsulinemia, insulin resistance, and hepatic steatosis in vivo . Based on the hepatic metabolomic analysis results, alterations in metabolites associated with pathological changes were examined. A total of 194 identified metabolites were mapped to 46 relative metabolic pathways, including those of energy metabolism. In addition, via in silico profiling for secondary maca metabolites by a joint pharmacophore- and structure-based approach, a compound-target-disease network was established. The results revealed that 32 bioactive compounds in maca targeted 16 proteins involved in metabolism disorder. Considering the combined metabolomics and virtual screening results, we employed quantitative real-time PCR assays to verify the gene expression of key enzymes in the relevant pathways. AEM promoted glycolysis and inhibited gluconeogenesis via regulating the expression of key genes such as Gck and Pfkm . Moreover, AEM upregulated tricarboxylic acid (TCA) cycle flux by changing the concentrations of intermediates and increasing the mRNA levels of Aco2 , Fh , and Mdh2 . In addition, the lipid-lowering effects of AEM in boththe serum and liver may be partly related to PPARα signaling activation, including enhanced fatty acid β-oxidation and lipogenesis pathway inhibition. Together, our data demonstrated that AEM intervention significantly improved lipid and glucose metabolism disorder by regulating the glycolysis/gluconeogenesis-TCA cycle and by modulating gene expression levels involved in the PPARα signaling pathway.
机译:玛卡(Lepidium meyenii Walpers)被用作膳食补充剂和民族药。近年来,由于玛咖具有多种生物活性,它已成为世界范围内备受瞩目的功能食品。这项研究是第一项探索性研究,旨在研究黑玛卡(AEM)水提取物对高脂,高果糖饮食(HFD)诱导的金仓鼠新陈代谢障碍的预防和改善能力,并确定其中的潜在机制在这些效果。在20周内,分别给6周龄的雄性金黄仓鼠喂食以下食物:(1)标准饮食,(2)HFD,(3)补充二甲双胍的HFD或(4)补充三剂AEM的HFD (300、600或1,200 mg / kg)。 20周后,每天接受AEM补充的金色仓鼠在体内具有改善高脂血症,高胰岛素血症,胰岛素抵抗和肝脂肪变性的有益作用。根据肝脏代谢组学分析结果,研究了与病理变化相关的代谢物变化。总共194种已鉴定的代谢物被映射到46种相对代谢途径,包括能量代谢途径。另外,通过基于联合药效团和基于结构的方法对次要玛咖代谢产物进行计算机分析,建立了化合物-靶标-疾病网络。结果表明,玛咖中的32种生物活性化合物靶向与代谢异常有关的16种蛋白质。考虑到组合的代谢组学和虚拟筛选结果,我们采用了定量实时PCR分析法来验证相关途径中关键酶的基因表达。 AEM通过调节Gck和Pfkm等关键基因的表达促进糖酵解和抑制糖异生。此外,AEM通过改变中间体的浓度并增加Aco2,Fh和Mdh2的mRNA水平来上调三羧酸(TCA)循环通量。此外,AEM在血清和肝脏中的降脂作用可能部分与PPARα信号激活有关,包括增强的脂肪酸β-氧化和脂肪生成途径抑制。总之,我们的数据表明AEM干预可通过调节糖酵解/糖异生-TCA周期并调节PPARα信号通路中涉及的基因表达水平来显着改善脂质和葡萄糖代谢紊乱。

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