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Renal Acid-Base Physiology: Response of the mitochondrial proteome of rat renal proximal convoluted tubules to chronic metabolic acidosis

机译:肾酸碱生理学:大鼠肾脏近曲小管的线粒体蛋白质组对慢性代谢性酸中毒的反应

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摘要

Metabolic acidosis is a common clinical condition that is caused by a decrease in blood pH and bicarbonate concentration. Increased extraction and mitochondrial catabolism of plasma glutamine within the renal proximal convoluted tubule generates ammonium and bicarbonate ions that facilitate the excretion of acid and partially restore acid-base balance. Previous studies identified only a few mitochondrial proteins, including two key enzymes of glutamine metabolism, which are increased during chronic acidosis. A workflow was developed to characterize the mitochondrial proteome of the proximal convoluted tubule. Based upon the increase in specific activity of cytochrome c oxidase, the isolated mitochondria were enriched eightfold. Two-dimensional liquid chromatography coupled with mass spectrometry was utilized to compare mitochondrial-enriched samples from control and chronic acidotic rats. Proteomic analysis identified 901 proteins in the control and acidotic samples. Further analysis identified 37 peptides that contain an N-ε-acetyl-lysine; of these, 22 are novel sites. Spectral counting analysis revealed 33 proteins that are significantly altered in abundance in response to chronic metabolic acidosis. Western blot analysis was performed to validate the calculated changes in abundance. Thus the current study represents the first comprehensive analysis of the mitochondrial proteome of the rat renal proximal convoluted tubule and its response to metabolic acidosis.
机译:代谢性酸中毒是一种常见的临床疾病,由血液pH值和碳酸氢盐浓度降低引起。肾近曲小管内血浆谷氨酰胺的提取和线粒体分解代谢增加,产生铵离子和碳酸氢根离子,促进酸的排泄并部分恢复酸碱平衡。先前的研究仅发现了少数线粒体蛋白,包括两种谷氨酰胺代谢关键酶,这些蛋白在慢性酸中毒时会增加。开发了一种工作流程来表征近端曲折小管的线粒体蛋白质组。基于细胞色素C氧化酶比活性的增加,分离的线粒体富集了八倍。二维液相色谱与质谱联用用于比较对照和慢性酸中毒大鼠的线粒体富集样品。蛋白质组学分析在对照和酸中毒样品中鉴定出901种蛋白质。进一步的分析鉴定出37种含有N-ε-乙酰赖氨酸的肽。其中22个是新颖的网站。光谱计数分析显示33种蛋白质在响应慢性代谢性酸中毒后其丰度发生了显着变化。进行蛋白质印迹分析以验证计算的丰度变化。因此,本研究代表了对大鼠肾脏近曲小管的线粒体蛋白质组及其对代谢性酸中毒反应的首次综合分析。

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