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Chlorogenic acids inhibit glutamate dehydrogenase and decrease intracellular ATP levels in cultures of chick embryo retina cells

机译:绿原酸抑制谷氨酸脱氢酶并降低鸡胚胚胎视网膜细胞培养物中的细胞内ATP水平

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Chlorogenic acids (CGAs) are a group of phenolic compounds found in worldwide consumed beverages such as coffee and green tea. They are synthesized from an esterification reaction between cinnamic acids, including caffeic (CFA), ferulic and p-coumaric acids with quinic acid (QA), forming several mono- and di-esterified isomers. The most prevalent and studied compounds are 3-O-caffeoylquinic acid (3-CQA), 4-O-caffeoylquinic acid (4-CQA) and 5-O-caffeoylquinic acid (5-CQA), widely described as having antioxidant and cell protection effects. CGAs can also modulate glutamate release from microglia by a mechanism involving a decrease of reactive oxygen species (ROS). Increased energy metabolism is highly associated with enhancement of ROS production and cellular damage. Glutamate can also be used as an energy source by glutamate dehydrogenase (GDH) enzyme, providing α-ketoglutarate to the tricarboxylic acid (TCA) cycle for ATP synthesis. High GDH activity is associated with some disorders, such as schizophrenia and hyperinsulinemia/hyperammonemia syndrome. In line with this, our objective was to investigate the effect of CGAs on GDH activity. We show that CGAs and CFA inhibits GDH activity in dose-dependent manner, reaching complete inhibition at high concentration with IC50 of 52?μM for 3-CQA and 158.2?μM for CFA. Using live imaging confocal microscopy and microplate reader, we observed that 3-CQA and CFA can be transported into neuronal cells by an Na+-dependent mechanism. Moreover, neuronal cells treated with CGAs presented lower intracellular ATP levels. Overall, these data suggest that CGAs have therapeutic potential for treatment of disorders associated with high GDH activity.
机译:绿原酸(CGA)是一组在全球消耗的饮料中发现的酚类化合物,如咖啡和绿茶。它们由肉桂酸(Caffeic(CFA),含有醋酸(CFA),阿魏和对香豆酸的酯化反应合成,形成几种单酯和二酯化异构体。最普遍和研究的化合物是3-O-咖啡算法(3-CQA),4-O-咖啡酸(4-CQA)和5-O-咖啡算法(5-CQA),广泛描述为具有抗氧化和细胞保护效果。 CGA还可以通过涉及反应性氧物质(ROS)减少的机制来调节从小胶质细胞的谷氨酸释放。增加的能量代谢与增强ROS生产和细胞损伤高度相关。谷氨酸还可以用谷氨酸脱氢酶(GDH)酶用作能源,为ATP合成提供α-酮戊酸(TCA)循环。高GDH活性与某些疾病有关,例如精神分裂症和高胰岛素血症/高胰症症综合征。符合这一点,我们的目标是调查CGA对GDH活动的影响。我们表明CGA和CFA以剂量依赖性方式抑制GDH活性,高浓度达到完全抑制,IC50为52Ω·μm,对于CFA,158.2μm。使用实时成像共焦显微镜和微孔板读者,我们观察到3-CQA和CFA可以通过NA +依赖性机制传送到神经元细胞中。此外,用CGA处理的神经元细胞呈现较低的细胞内ATP水平。总体而言,这些数据表明CGA具有治疗与高GDH活性相关的病症的治疗潜力。

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