首页> 美国卫生研究院文献>American Journal of Physiology - Renal Physiology >pH-responsive gluconeogenic renal epithelial LLC-PK1-FBPase+cells: a versatile in vitro model to study renal proximal tubule metabolism and function
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pH-responsive gluconeogenic renal epithelial LLC-PK1-FBPase+cells: a versatile in vitro model to study renal proximal tubule metabolism and function

机译:pH响应糖原性肾上皮LLC-PK1-FBPase +细胞:研究肾近端小管代谢和功能的多功能体外模型

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摘要

Ammoniagenesis and gluconeogenesis are prominent metabolic features of the renal proximal convoluted tubule that contribute to maintenance of systemic acid-base homeostasis. Molecular analysis of the mechanisms that mediate the coordinate regulation of the two pathways required development of a cell line that recapitulates these features in vitro. By adapting porcine renal epithelial LLC-PK1 cells to essentially glucose-free medium, a gluconeogenic subline, termed LLC-PK1-FBPase+ cells, was isolated. LLC-PK1-FBPase+ cells grow in the absence of hexoses and pentoses and exhibit enhanced oxidative metabolism and increased levels of phosphate-dependent glutaminase. The cells also express significant levels of the key gluconeogenic enzymes, fructose-1,6-bisphosphatase (FBPase) and phosphoenolpyruvate carboxykinase (PEPCK). Thus the altered phenotype of LLC-PK1-FBPase+ cells is pleiotropic. Most importantly, when transferred to medium that mimics a pronounced metabolic acidosis (9 mM HCO3, pH 6.9), the LLC-PK1-FBPase+ cells exhibit a gradual increase in NH4+ ion production, accompanied by increases in glutaminase and cytosolic PEPCK mRNA levels and proteins. Therefore, the LLC-PK1-FBPase+ cells retained in culture many of the metabolic pathways and pH-responsive adaptations characteristic of renal proximal tubules. The molecular mechanisms that mediate enhanced expression of the glutaminase and PEPCK in LLC-PK1-FBPase+ cells have been extensively reviewed. The present review describes novel properties of this unique cell line and summarizes the molecular mechanisms that have been defined more recently using LLC-PK1-FBPase+ cells to model the renal proximal tubule. It also identifies future studies that could be performed using these cells.
机译:氨生成和糖异生是肾脏近端曲折小管的突出代谢特征,有助于维持全身性酸碱稳态。对介导这两个途径的协调调节的机制进行分子分析需要开发一种在体外概括这些特征的细胞系。通过使猪肾上皮LLC-PK1细胞适应基本无葡萄糖的培养基,分离出称为LLC-PK1-FBPase + 细胞的糖原异生亚系。 LLC-PK1-FBPase + 细胞在不存在己糖和戊糖的情况下生长,并表现出增强的氧化代谢和磷酸依赖性谷氨酰胺酶水平。这些细胞还表达大量的关键糖异生酶,果糖-1,6-双磷酸酶(FBPase)和磷酸烯醇丙酮酸羧激酶(PEPCK)。因此,LLC-PK1-FBPase + 细胞的表型改变是多效的。最重要的是,当转移至模拟明显的代谢性酸中毒(9 mM HCO3 -,pH 6.9)的培养基中时,LLC-PK1-FBPase + 细胞的分泌逐渐增加。 NH4 + 离子的产生,伴随着谷氨酰胺酶和胞质PEPCK mRNA水平和蛋白质的增加。因此,LLC-PK1-FBPase + 细胞保留在肾近端小管的许多代谢途径和pH响应适应性中。广泛研究了介导LLC-PK1-FBPase + 细胞中谷氨酰胺酶和PEPCK表达增强的分子机制。本文综述了这种独特细胞系的新颖特性,并总结了最近使用LLC-PK1-FBPase + 细胞对肾小管进行建模的分子机制。它还确定了可以使用这些细胞进行的未来研究。

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