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无限顺式动力学支持红细胞葡萄糖转运的载体模型。

Infinite-cis kinetics support the carrier model for erythrocyte glucose transport.

作者信息

Wheeler T J, Whelan J D

机构信息

Department of Biochemistry, University of Louisville School of Medicine, Kentucky 40292.

出版信息

Biochemistry. 1988 Mar 8;27(5):1441-50. doi: 10.1021/bi00405a008.

Abstract

It has been claimed that the Km for infinite-cis uptake of glucose in human erythrocytes is so low that the carrier model for transport must be rejected. We redetermined this parameter for three experimental conditions and found instead that the Km values were in good agreement with the model. For each of a variety of cis glucose concentrations, cells were preequilibrated with various concentrations of glucose, and the apparent Km was determined as the intracellular concentration reducing the initial rate of net uptake by half. The dependence of the apparent Km values on the cis glucose was as predicted by the carrier model; the infinite-cis Km was determined from both this concentration dependence and the extrapolated value at infinite cis glucose. The resulting values were 15 mM for fresh blood at 0 degrees C, 39 mM for outdated blood at 0 degrees C, and 11 mM for outdated blood at 25 degrees C. Previous measurements of the Km at room temperature yielded values of 2-3 mM. These earlier studies used a time course procedure that indicated rapid changes in rates during the initial 10 s of uptake but did not directly measure such changes. We examined the uptake of 60 mM glucose at 20 degrees C into cells containing 0 and 5 mM glucose; rapid changes in rates were not observed in the first few seconds, and the time courses were more consistent with our higher Km values. Our new values, together with other initial rate measurements in the literature, support the adequacy of the carrier model to account for the kinetics of glucose transport in human erythrocytes.

摘要

有人声称,人类红细胞中葡萄糖无限顺式摄取的米氏常数(Km)非常低,以至于必须摒弃载体运输模型。我们在三种实验条件下重新测定了该参数,结果发现Km值与该模型吻合良好。对于各种顺式葡萄糖浓度,细胞先用不同浓度的葡萄糖进行预平衡,表观Km被确定为使净摄取初始速率减半的细胞内浓度。表观Km值对顺式葡萄糖的依赖性正如载体模型所预测的那样;无限顺式Km是根据这种浓度依赖性以及无限顺式葡萄糖时的外推值确定的。结果值分别为:0℃时新鲜血液为15 mM,0℃时陈旧血液为39 mM,25℃时陈旧血液为11 mM。之前在室温下对Km的测量得出的值为2 - 3 mM。这些早期研究采用了一种时间进程程序,该程序表明摄取最初10秒内速率有快速变化,但未直接测量此类变化。我们研究了20℃时60 mM葡萄糖进入含有0和5 mM葡萄糖的细胞的摄取情况;在最初几秒内未观察到速率的快速变化,时间进程与我们较高的Km值更为一致。我们的新值,连同文献中的其他初始速率测量结果,支持载体模型足以解释人类红细胞中葡萄糖运输的动力学。

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