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载体介导的大鼠肝细胞对乳酸的摄取。pH的影响及L-乳酸转运的可能机制。

Carrier-mediated uptake of lactate in rat hepatocytes. Effects of pH and possible mechanisms for L-lactate transport.

作者信息

Fafournoux P, Demigné C, Rémésy C

出版信息

J Biol Chem. 1985 Jan 10;260(1):292-9.

PMID:3965451
Abstract

The rate of uptake and the distribution ratio between intra- and extracellular compartments of L- and D-lactate were studied in hepatocyte preparations from fed rats. L- and D-lactate uptake apparently depended on both passive diffusion and carrier-mediated components. The apparent Km of the high-affinity carrier for L-lactate was in the range of 1.8 mM. The reciprocal competitive inhibitions between isomers of lactate suggest that L- and D-lactate might be transported by distinct carriers. Lactate transport was inhibited by various anions; pyruvate was the most potent anion, whereas only high concentrations of ketone bodies were effective. Acidic extracellular pH enhanced lactate uptake, this effect being more pronounced for L-lactate. At low pH, L-lactate was concentrated into hepatocytes, but its affinity for the carrier appeared unchanged, suggesting the existence of a process gaining energy from the pH gradient across the cell membrane. In the hypothesis of a lactate/H+ symport, the affinity for H+ was not dependent on lactate concentration and the apparent Km for H+ corresponded to a pH of 7.34. No trans-stimulation of lactate uptake after prior loading of the cells with pyruvate or lactate was observed. The present data suggest that, at physiological concentrations, lactate uptake by the liver might be largely carrier-mediated and the rate of transport across the liver cell membrane may be of a magnitude relatively comparable to the rate of metabolism.

摘要

在喂食大鼠的肝细胞制剂中,研究了L-乳酸和D-乳酸的摄取速率以及细胞内和细胞外区室之间的分布比例。L-乳酸和D-乳酸的摄取显然取决于被动扩散和载体介导的成分。L-乳酸高亲和力载体的表观Km在1.8 mM范围内。乳酸异构体之间的相互竞争性抑制表明L-乳酸和D-乳酸可能由不同的载体转运。乳酸转运受到各种阴离子的抑制;丙酮酸是最有效的阴离子,而只有高浓度的酮体才有效。细胞外酸性pH增强了乳酸摄取,这种效应在L-乳酸中更为明显。在低pH下,L-乳酸被浓缩到肝细胞中,但其对载体的亲和力似乎没有变化,这表明存在一种从跨细胞膜的pH梯度获取能量的过程。在乳酸/H+同向转运的假设中,对H+的亲和力不依赖于乳酸浓度,H+的表观Km对应于pH 7.34。在用丙酮酸或乳酸预先加载细胞后,未观察到乳酸摄取的转刺激作用。目前的数据表明,在生理浓度下,肝脏对乳酸的摄取可能主要由载体介导,并且跨肝细胞膜的转运速率可能与代谢速率在数量上相对相当。

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