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兔膀胱顶端膜的通透性及钠泵的动力学特性

Apical membrane permeability and kinetic properties of the sodium pump in rabbit urinary bladder.

作者信息

Lewis S A, Wills N K

出版信息

J Physiol. 1983 Aug;341:169-84. doi: 10.1113/jphysiol.1983.sp014799.

Abstract

Previous studies have shown that aldosterone stimulates the rate of Na+ transport across the rabbit urinary bladder epithelium by increasing the apical membrane permeability to Na+. Paradoxically, ion-sensitive and conventional micro-electrode measurements demonstrated that intracellular Na+ activity aiNa+ was essentially unchanged by aldosterone, i.e. aiNa+ was constant regardless of the rate of Na+ transport. The present study was designed to resolve this apparent contradiction. The effects of elevated, endogenous aldosterone levels produced by low-Na+ diet (Lewis & Diamond, 1976) on urinary bladder Na+ transport were investigated in vitro using Ussing-type chambers and intracellular conventional and ion-sensitive microelectrodes. Apical membrane selectivity and kinetics of the Na+ pump were assessed as a function of hormone stimulation. The aldosterone-stimulated increase in Na+ transport was accounted for by increases in both the relative selective permeability of the apical membrane to Na+ and an increase in its absolute Na+ permeability. The kinetics of the Na+ pump were evaluated electrically by loading the cells with Na+ (monitored with Na+-sensitive micro-electrodes) or alternatively by manipulating serosal solution K+ concentration and measuring changes in the basolateral membrane electromotive forces and resistance. From these measurements the current generated by the pump was calculated as a function of intracellular Na+ or extracellular K+. The kinetics of the pump were not altered by aldosterone. A model of highly co-operative binding estimated Km for Na+ as 14.2 mM and 2.3 mM for K+. Hill coefficients for these ions were 2.8 and 1.8, respectively, consistent with a pump stoichiometry of 3 Na+ to 2 K+. The kinetic properties of the Na-K pump indicate that physiological levels of aiNa+ are poised at the foot of a step kinetic curve which energetically favours Na+ extrusion.

摘要

以往的研究表明,醛固酮通过增加顶端膜对Na+的通透性来刺激兔膀胱上皮细胞的Na+转运速率。矛盾的是,离子敏感和传统微电极测量表明,醛固酮对细胞内Na+活性aiNa+基本没有影响,即无论Na+转运速率如何,aiNa+都是恒定的。本研究旨在解决这一明显的矛盾。采用Ussing型小室以及细胞内传统和离子敏感微电极,在体外研究了低钠饮食(Lewis和Diamond,1976)导致的内源性醛固酮水平升高对膀胱Na+转运的影响。评估了顶端膜的选择性以及Na+泵的动力学作为激素刺激的函数。醛固酮刺激引起的Na+转运增加是由于顶端膜对Na+的相对选择性通透性增加以及其绝对Na+通透性增加所致。通过用Na+加载细胞(用Na+敏感微电极监测),或者通过操纵浆膜溶液K+浓度并测量基底外侧膜电动势和电阻的变化,用电学方法评估Na+泵的动力学。根据这些测量结果,计算出泵产生的电流作为细胞内Na+或细胞外K+的函数。醛固酮并未改变泵的动力学。一个高度协同结合的模型估计Na+的Km为14.2 mM,K+的Km为2.3 mM。这些离子的希尔系数分别为2.8和1.8,与3个Na+对2个K+的泵化学计量比一致。Na-K泵的动力学特性表明,生理水平的aiNa+处于阶梯动力学曲线的底部,这在能量上有利于Na+的排出。

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