温度与张力对犬红细胞阳离子转运的相互作用。

Interactions between temperature and tonicity on cation transport in dog red cells.

作者信息

Elford B C

出版信息

J Physiol. 1975 Mar;246(2):371-95. doi: 10.1113/jphysiol.1975.sp010895.

DOI:10.1113/jphysiol.1975.sp010895

PMID:806680

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1309423/

Abstract

The temperature-dependence of the uptake of 24Na and 42K into dog red cells between 38 and 4 degrees C has been investigated. The effects on the cation fluxes of partial dehydration of the cells in hyperosmolar sucrose (50-125 mM) have also been studied. 2. A Hamilton gas-tight syringe was used to pipette accurately reproducible volumes of packed cells which contained in addition to 24Na or 42K either [131I]albumin or [51Cr]EDTA as extracellular markers. 3. At 38 degrees C Na flux (m-equiv/l. isosmolar cell volume. hr) increased from 2-8 +/- 0-1 (n = 8) in cells of normal volume to 226 +/- 8 (n = 8) when the cells were shrunken by 27-4 +/- 0-6% (n = 8) in media containing sucrose (100 mM). K influx remained relatively constant under these conditions. 4. The exchange of 24Na in shrunken cells followed a single exponential time course but about 9% of the intracellular Na apparently did not exchange with 24Na in the bathing medium. 5. The steady-state influx of Na in cells of normal volume was maximal at about 22 degrees C. The temperature dependence of the Na fluxes in shrunken cells was described by an Arrhenius relationship with a change in slope at about 22 degrees C. 6. The K influx in cells of normal volume decreased as the temperature was lowered from 38 degrees C, to about 12 degrees C, at which temperature the flux was at a well defined minimum. Above 12 degrees C, cell shrinkage had hardly any effect on K influx, but below 12 degrees C the influx in shrunken cells was significantly less than in cells of normal volume. 7. The selective increase in Na flux induced by cell shrinkage results from a Na:Na exchange process which cannot be explained in terms of Ussing's (1947) model of carrier-mediated exchange diffusion. 8. The lack of coupling between the effects of temperature and cell volume on the fluxes of Na and K indicates that localized structural changes of lipid-protein complexes specific for Na or K are responsible for the cation transport characteristics of dog red cells, and that phase transitions in the lipids of the cell membrane are unlikely to account for the temperature dependence of the fluxes.

摘要

研究了38℃至4℃之间狗红细胞对24Na和42K摄取的温度依赖性。还研究了高渗蔗糖（50 - 125 mM）中细胞部分脱水对阳离子通量的影响。2. 使用汉密尔顿气密注射器精确吸取可重复的红细胞体积，这些红细胞除了含有24Na或42K外，还含有[131I]白蛋白或[51Cr]EDTA作为细胞外标志物。3. 在38℃时，正常体积细胞的Na通量（毫当量/升等渗细胞体积·小时）从2 - 8±0 - 1（n = 8）增加到当细胞在含蔗糖（100 mM）的培养基中收缩27 - 4±0 - 6%（n = 8）时的226±8（n = 8）。在这些条件下，K流入量保持相对恒定。4. 收缩细胞中24Na的交换遵循单一指数时间进程，但约9%的细胞内Na显然未与浴液中的24Na交换。5. 正常体积细胞中Na的稳态流入在约22℃时最大。收缩细胞中Na通量的温度依赖性由阿伦尼乌斯关系描述，在约22℃时斜率发生变化。6. 正常体积细胞中的K流入量随着温度从38℃降低到约12℃而减少，在该温度下通量处于明确的最小值。高于12℃时，细胞收缩对K流入量几乎没有影响，但低于12℃时，收缩细胞中的流入量明显低于正常体积细胞。7. 细胞收缩诱导的Na通量选择性增加是由Na:Na交换过程引起的，这无法用乌辛（1947年）的载体介导交换扩散模型来解释。8. 温度和细胞体积对Na和K通量的影响之间缺乏耦合表明，狗红细胞阳离子转运特性是由Na或K特异性的脂 - 蛋白复合物的局部结构变化引起的，并且细胞膜脂质的相变不太可能解释通量的温度依赖性。