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大鼠淋巴细胞中氯离子跨膜分布的决定因素:Cl(-)-HCO3-交换的作用

Determinants of the transmembrane distribution of chloride in rat lymphocytes: role of Cl(-)-HCO3- exchange.

作者信息

Garcia-Soto J J, Grinstein S

机构信息

Instituto de Investigacion en Biologia Experimental, Facultat de Quimica, Universidad de Guanajuato, Mexico.

出版信息

Am J Physiol. 1990 Jun;258(6 Pt 1):C1108-16. doi: 10.1152/ajpcell.1990.258.6.C1108.

DOI:10.1152/ajpcell.1990.258.6.C1108
PMID:2163199
Abstract

The purpose of the present experiments was to establish the factors that determine the intracellular Cl- concentration ([Cl-]i) of lymphocytes. Coulometric and isotope equilibration determinations indicated that [Cl-]i was in the range of 70-85 mmol/l cells. Since the membrane potential (Em) of these cells approximates -55 mV, [Cl-]i is severalfold higher than the level expected at electrochemical equilibrium (approximately 16 mM). This suggests that conductive pathways contribute marginally to the distribution of Cl-. Accordingly, altering the force driving conductive Cl- fluxes by manipulating Em had little effect on [Cl-]i. The possible role of electroneutral cation-Cl- cotransport in the accumulation of intracellular Cl- was also assessed. 36Cl- uptake was largely unaffected by omission of extracellular Na+ and K+ or by addition of bumetanide, a potent cotransport inhibitor. Moreover, [Cl-]i remained unaltered for at least 1 h in cells incubated without Na+ or K+ or in the presence of loop diuretics. Thus it appears unlikely that Cl(-)-anion cotransport plays a major role in maintaining [Cl-]i. A vigorous stilbene disulfonate-sensitive anion exchanger was detected in thymocytes. This system constitutes a large fraction of the Cl- flux pathways and is possibly a major contributor to the establishment of [Cl-]i. Accordingly, modifying the force driving Cl- through the exchanger, by altering pH at constant PCO2, resulted in changes in cellular Cl- content and associated changes in cell volume. These effects were markedly reduced in the nominal absence of HCO3- or in the presence of disulfonic stilbene derivatives, suggesting that they are mediated by Cl(-)-HCO3- exchange.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

本实验的目的是确定决定淋巴细胞细胞内氯离子浓度([Cl-]i)的因素。电量分析法和同位素平衡测定表明,[Cl-]i在70 - 85 mmol/l细胞范围内。由于这些细胞的膜电位(Em)接近 -55 mV,[Cl-]i比电化学平衡时预期的水平(约16 mM)高几倍。这表明导电途径对Cl-的分布贡献很小。因此,通过操纵Em改变驱动导电Cl-通量的力对[Cl-]i影响不大。还评估了电中性阳离子 - Cl-共转运在细胞内Cl-积累中的可能作用。细胞外Na+和K+的缺失或强效共转运抑制剂布美他尼的添加对36Cl-摄取的影响不大。此外,在无Na+或K+孵育的细胞中或在存在襻利尿剂的情况下,[Cl-]i至少1小时保持不变。因此,Cl(-)-阴离子共转运似乎不太可能在维持[Cl-]i中起主要作用。在胸腺细胞中检测到一种活性的对二苯乙烯二磺酸盐敏感的阴离子交换器。该系统构成了Cl-通量途径的很大一部分,并且可能是[Cl-]i建立的主要贡献者。因此,在恒定PCO2下通过改变pH来改变驱动Cl-通过交换器的力,会导致细胞Cl-含量的变化以及细胞体积的相关变化。在名义上不存在HCO3-或存在二苯乙烯二磺酸衍生物的情况下,这些效应明显降低,表明它们是由Cl(-)-HCO3-交换介导的。(摘要截短于250字)

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