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家兔肾近端小管中的钾转运:钡、哇巴因、缬氨霉素及其他离子载体的作用

Potassium transport in the rabbit renal proximal tubule: effects of barium, ouabain, valinomycin, and other ionophores.

作者信息

Soltoff S P, Mandel L J

出版信息

J Membr Biol. 1986;94(2):153-61. doi: 10.1007/BF01871195.

Abstract

Potassium fluxes in a suspension of rabbit proximal tubules were monitored using a potassium-sensitive extracellular electrode. Ouabain (10(-4) M) and barium (5 mM) were used to selectively quantitate the potassium efflux pathway (105 +/- 5 nmol K+ X mg protein-1 X min-1) and the sodium pump-related potassium influx (108 +/- 7), respectively. These equal and opposite fluxes suggest that potassium accumulation in the cell occurs mainly through the sodium pump and that potassium efflux occurs mainly through barium-sensitive potassium channels. Thus the activity of the sodium pump (Na,K-ATPase) in the basolateral membrane of the proximal tubule is balanced by the efflux of potassium, presumably across the basolateral membrane, which has a high potassium permeability. In addition, the effect of valinomycin and other ionophores was examined on potassium fluxes and several metabolic parameters [oxygen consumption (QO2), ATP content]. The addition of valinomycin to the tubules produced a net efflux of potassium which was quantitatively equivalent to the efflux produced by the addition of ouabain. The valinomycin-induced efflux was mainly due to the activity of valinomycin as a mitochondrial uncoupler, which indirectly inhibited the sodium pump by allowing a rapid reduction of the intracellular ATP. Amphotericin, nystatin, and monensin all produced large net releases of intracellular potassium. The action of the ionophores could be localized to the plasma or mitochondrial membrane and classified into three groups, as follows: those which demonstrated full mitochondrial uncoupler activity (FCCP, valinomycin), those which had no uncoupler activity (amphotericin B, nystatin); and those which displayed partial uncoupler activity (monensin, nigericin).

摘要

使用钾敏感型细胞外电极监测兔近端小管悬浮液中的钾通量。哇巴因(10⁻⁴ M)和钡(5 mM)分别用于选择性定量钾外流途径(105±5 nmol K⁺×mg蛋白⁻¹×min⁻¹)和与钠泵相关的钾内流(108±7)。这些大小相等且方向相反的通量表明,细胞内钾的积累主要通过钠泵发生,而钾外流主要通过对钡敏感的钾通道发生。因此,近端小管基底外侧膜中钠泵(Na,K - ATP酶)的活性由钾外流平衡,推测钾外流是通过具有高钾通透性的基底外侧膜进行的。此外,还研究了缬氨霉素和其他离子载体对钾通量和几个代谢参数[耗氧量(QO₂)、ATP含量]的影响。向小管中添加缬氨霉素会产生钾的净外流,其数量上等同于添加哇巴因所产生的外流。缬氨霉素诱导的外流主要是由于缬氨霉素作为线粒体解偶联剂的活性,它通过使细胞内ATP迅速减少而间接抑制钠泵。两性霉素、制霉菌素和莫能菌素都会导致细胞内钾的大量净释放。离子载体的作用可定位于质膜或线粒体膜,并分为以下三组:表现出完全线粒体解偶联活性的(FCCP、缬氨霉素),没有解偶联活性的(两性霉素B、制霉菌素);以及表现出部分解偶联活性的(莫能菌素、尼日利亚菌素)。

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