Scaduto R C, Davis E J
Biochem J. 1986 Aug 1;237(3):691-8. doi: 10.1042/bj2370691.
The metabolism of glycerate and aspartate was investigated in perfused rat kidneys. The major pathway active for aspartate metabolism and NH3 production was found to include transamination, and not the purine nucleotide cycle. Pyruvate cycling was identified as a means by which reducing potential is generated in the cytosol for glucose and lactate production from these substrates. Inhibition of mitochondrial pyruvate transport caused an inhibition of glucose production, accumulation of lactate and pyruvate in the perfusate, and a decrease in the [lactate]/[pyruvate] ratio in kidneys perfused with aspartate. These data indicate a role of mitochondrial pyruvate transport in the provision of cytosolic reducing potential. With either aspartate or glycerate, 3-mercaptopicolinic acid (3-MPA) suppressed glucose synthesis and caused accumulation of malate plus fumarate within the kidney. Glucose production from glycerate was much less sensitive to the presence of 3-MPA than was glucose production from aspartate, illustrating a phosphoenolpyruvate carboxykinase (PEPCK)-independent pathway for the cycling of pyruvate. In aspartate-perfused kidneys, the presence of 3-MPA, at concentrations that completely blocked glucose accumulation in the perfusate, did not affect the rate of NH3 production and had only a minor effect on the rate of aspartate uptake. These data allow for an estimation of the rate of pyruvate formation from aspartate of about 1 mumol/min per kidney under conditions of complete PEPCK inhibition. Thus a PEPCK-independent pathway is operative for amino acid oxidation and pyruvate formation in perfused kidneys. The NADP-linked, but not the NAD-linked, 'malic' enzyme activity of the kidney cortex was found to be sufficient to catalyse this estimated rate of pyruvate formation.
在灌注大鼠肾脏中研究了甘油酸和天冬氨酸的代谢。发现天冬氨酸代谢和氨生成的主要活性途径包括转氨作用,而非嘌呤核苷酸循环。丙酮酸循环被确定为一种在细胞质中产生还原电位以从这些底物生成葡萄糖和乳酸的方式。线粒体丙酮酸转运的抑制导致葡萄糖生成受到抑制、灌注液中乳酸和丙酮酸积累,以及在灌注天冬氨酸的肾脏中[乳酸]/[丙酮酸]比值降低。这些数据表明线粒体丙酮酸转运在提供细胞质还原电位方面的作用。使用天冬氨酸或甘油酸时,3-巯基吡啶甲酸(3-MPA)抑制葡萄糖合成并导致肾脏内苹果酸加富马酸积累。甘油酸生成葡萄糖对3-MPA的存在比天冬氨酸生成葡萄糖的敏感性低得多,这说明了丙酮酸循环的一条不依赖磷酸烯醇式丙酮酸羧激酶(PEPCK)的途径。在灌注天冬氨酸的肾脏中,3-MPA的存在(其浓度完全阻断灌注液中的葡萄糖积累)并不影响氨生成速率,对天冬氨酸摄取速率仅有轻微影响。这些数据使得在完全PEPCK抑制条件下,能够估计每个肾脏中天冬氨酸生成丙酮酸的速率约为1 μmol/分钟。因此,一条不依赖PEPCK的途径在灌注肾脏的氨基酸氧化和丙酮酸形成中起作用。发现肾皮质中与NADP相关而非与NAD相关的“苹果酸”酶活性足以催化该估计的丙酮酸形成速率。