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首页> 外文期刊>Journal of cellular biochemistry. >Potential role of branched-chain amino acids in glucose metabolism through the accelerated induction of the glucose-sensing apparatus in the liver.
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Potential role of branched-chain amino acids in glucose metabolism through the accelerated induction of the glucose-sensing apparatus in the liver.

机译:支链氨基酸通过加速肝脏中葡萄糖传感装置的诱导在葡萄糖代谢中的潜在作用。

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Branched-chain amino acids (BCAAs) have a potential to improve glucose metabolism in cirrhotic patients; however, the contribution of liver in this process has not been clarified. To estimate the effect of BCAA on glucose metabolism in liver, we evaluated the mRNA expression levels of glucose-sensing apparatus genes in HepG2 cells and in rat liver after oral administration of BCAA. HepG2 cells were cultured in low glucose (100 mg/dl) or high glucose (400 mg/dl) in the absence or presence of BCAA. The mRNA expression levels and protein levels of GLUT2 and liver-type glucokinase (L-GK) were estimated using RT-PCR and immunoblotting. The expression levels of transcriptional factors, including SREBP-1c, ChREBP, PPAR-gammam and LXRalpha, were estimated. The mRNA expression levels of transcriptional factors, glycogen synthase, and genes involved in gluconeogenesis were evaluated in rat liver at 3 h after the administration of BCAA. BCAA accelerated the expression of GLUT2 and L-GK in HepG2 cells in high glucose. Expression levels of ChREBP, SREBP-1c, and LXRalpha were also increased in this condition. BCAA administration enhanced the mRNA expression levels of L-GK, SREBP-1c, and LXRalpha and suppressed the expression levels of G-6-Pase in rat liver, without affecting the expression levels of glycogen synthase or serum glucose concentrations. BCAA administration enhanced the bioactivity of the glucose-sensing apparatus, probably via the activation of a transcriptional mechanism, suggesting that these amino acids may improve glucose metabolism through the accelerated utility of glucose and glucose-6-phosphate in the liver.
机译:肝硬化患者中的支链氨基酸(BCAA)具有改善葡萄糖代谢的潜力。但是,肝脏在该过程中的作用尚未阐明。为了评估BCAA对肝脏葡萄糖代谢的影响,我们评估了口服BCAA后HepG2细胞和大鼠肝脏中葡萄糖传感装置基因的mRNA表达水平。在不存在或存在BCAA的情况下,在低葡萄糖(100 mg / dl)或高葡萄糖(400 mg / dl)中培养HepG2细胞。使用RT-PCR和免疫印迹法评估GLUT2和肝型葡萄糖激酶(L-GK)的mRNA表达水平和蛋白水平。估计包括SREBP-1c,ChREBP,PPAR-γ和LXRalpha在内的转录因子的表达水平。在给予BCAA 3小时后,在大鼠肝脏中评估了转录因子,糖原合酶和糖异生相关基因的mRNA表达水平。 BCAA促进高糖HepG2细胞中GLUT2和L-GK的表达。在这种情况下,ChREBP,SREBP-1c和LXRalpha的表达水平也增加了。施用BCAA可以提高大鼠肝脏中L-GK,SREBP-1c和LXRalpha的mRNA表达水平,并抑制G-6-Pase的表达水平,而不会影响糖原合酶的表达水平或血清葡萄糖浓度。 BCAA的给药可能通过激活转录机制来增强葡萄糖传感装置的生物活性,这表明这些氨基酸可以通过加速葡萄糖和肝脏中的6-磷酸葡萄糖的使用来改善葡萄糖的代谢。

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