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马红细胞中K(+)-Cl-协同转运的调节

Modulation of K(+)-Cl- cotransport in equine red blood cells.

作者信息

Gibson J S, Godart H, Ellory J C, Staines H, Honess N A, Cossins A R

机构信息

Department of Veterinary Preclinical Science, University of Liverpool.

出版信息

Exp Physiol. 1994 Nov;79(6):997-1009. doi: 10.1113/expphysiol.1994.sp003824.

Abstract

Potassium transport was measured in equine red blood cells, using 86Rb+ influx as a convenient assay. A significant component of volume- and pH-sensitive K(+)-Cl- cotransport to the overall K+ flux was observed in all blood samples studied, although fluxes were variable between animals, and within individuals when measured at intervals over a period of weeks. The aryloxyacetic acid [(dihydroindenyl)oxy]alkanoic acid (DIOA), at a final concentration of 100 microM, inhibited most (> 95%) of the Cl(-)-dependent K+ flux, and DIOA sensitivity was therefore used to define the activity of the K(+)-Cl- cotransport. K(+)-Cl- cotransport was also sensitive to protein phosphatase inhibition with calyculin A or okadaic acid, with inhibition constants of 9 +/- 1 nM for calyculin and about 100 nM for okadaic acid. Peak fluxes were observed at an external pH of 6.7-7.0, with inhibition at higher and lower values. Volume-sensitive K+ fluxes assayed in autologous plasma, controlled for osmolaity, pH and potassium concentration, were significantly lower (28 +/- 8% of control values, n = 6) than those measured in saline. This inhibition was mimicked by the culture medium RPMI, but disappeared following dialysis of the plasma. Phosphate (5.6 mM) inhibited volume-sensitive K+ fluxes by 48 +/- 2%, n = 3; no significant effect was observed by increasing external magnesium concentrations to 0.5 or 2 mM. Thus, inhibition by RPMI, but not that by plasma, may be due to phosphate. Finally, volume- and pH-sensitive K+ fluxes were sensitive to oxygen tension and were abolished reversibly by equilibrating solutions with nitrogen, as opposed to air. Use of solutions equilibrated with different values of Po2 may account for some of the variability in equine red blood cell KCl fluxes. The importance of these observations to equine red blood cell homeostasis and haemodynamics is discussed.

摘要

利用⁸⁶Rb⁺内流作为一种便捷的检测方法,对马红细胞中的钾转运进行了测量。在所研究的所有血样中,均观察到对总体钾通量而言,体积和pH敏感的K⁺-Cl⁻协同转运是一个重要组成部分,尽管不同动物之间以及在数周内定期测量时个体内部的通量存在差异。终浓度为100 μM的芳氧基乙酸[(二氢茚基)氧基]链烷酸(DIOA)抑制了大部分(>95%)依赖Cl⁻的钾通量,因此DIOA敏感性被用于定义K⁺-Cl⁻协同转运的活性。K⁺-Cl⁻协同转运也对用花萼海绵诱癌素A或冈田酸抑制蛋白磷酸酶敏感,花萼海绵诱癌素的抑制常数为9±1 nM,冈田酸约为100 nM。在外部pH为6.7 - 7.0时观察到峰值通量,在更高和更低的值时受到抑制。在控制了渗透压、pH和钾浓度的自体血浆中检测的体积敏感钾通量显著低于在盐水中测量的通量(为对照值的28±8%,n = 6)。这种抑制作用在培养基RPMI中也有体现,但血浆透析后抑制作用消失。磷酸盐(5.6 mM)使体积敏感钾通量降低了48±2%,n = 3;将外部镁浓度提高到0.5或2 mM未观察到显著影响。因此,RPMI的抑制作用而非血浆的抑制作用可能归因于磷酸盐。最后,体积和pH敏感的钾通量对氧张力敏感,通过用氮气而非空气平衡溶液可使其可逆地消除。使用用不同Po₂值平衡的溶液可能是马红细胞KCl通量存在一些变异性的部分原因。讨论了这些观察结果对马红细胞内环境稳定和血液动力学的重要性。

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