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钠/钾/氯耦合外流。鱿鱼巨轴突中的“反向”单向通量。

Coupled Na/K/Cl efflux. "Reverse" unidirectional fluxes in squid giant axons.

作者信息

Altamirano A A, Russell J M

出版信息

J Gen Physiol. 1987 May;89(5):669-86. doi: 10.1085/jgp.89.5.669.

Abstract

Studies of unidirectional Cl-, Na+, and K+ effluxes were performed on isolated, internally dialyzed squid giant axons. The studies were designed to determine whether the coupled Na/K/Cl co-transporter previously identified as mediating influxes (Russell. 1983. Journal of General Physiology. 81:909-925) could also mediate the reverse fluxes (effluxes). We found that 10 microM bumetanide blocked 7-8 pmol/cm2 X s of Cl- efflux from axons containing ATP, Na+, and K+. However, if any one of these solutes was removed from the internal dialysis fluid, Cl- efflux was reduced by 7-8 pmol/cm2 X s and the remainder was insensitive to bumetanide. About 5 pmol/cm2 X s of Na+ efflux was inhibited by 10 microM bumetanide in the continuous presence of 10(-5) M ouabain and 10(-7) M tetrodotoxin if Cl-, K+, and ATP were all present in the internal dialysis fluid. However, the omission of Cl- or K+ or ATP reduced the Na+ efflux, leaving it bumetanide insensitive. K+ efflux had to be studied under voltage-clamp conditions with the membrane potential held at -90 mV because the dominant pathway for K+ efflux (the delayed rectifier) has a high degree of voltage sensitivity. Under this voltage-clamped condition, 1.8 pmol/cm2 X s of K+ efflux could be inhibited by 10 microM bumetanide. All of these results are consistent with a tightly coupled Na/K/Cl co-transporting efflux mechanism. Furthermore, the requirements for cis-side co-ions and intracellular ATP are exactly like those previously described for the coupled Na/K/Cl influx process. We propose that the same transporter mediates both influx and efflux, hence demonstrating "reversibility," a necessary property for an ion-gradient-driven transport process.

摘要

对分离的、内部透析的枪乌贼巨大轴突进行了单向氯离子、钠离子和钾离子外流的研究。这些研究旨在确定先前鉴定为介导内流的钠/钾/氯协同转运体(Russell,1983年,《普通生理学杂志》,81:909 - 925)是否也能介导反向流动(外流)。我们发现,10微摩尔布美他尼可阻断含ATP、钠离子和钾离子的轴突中7 - 8皮摩尔/平方厘米·秒的氯离子外流。然而,如果从内部透析液中去除这些溶质中的任何一种,氯离子外流会减少7 - 8皮摩尔/平方厘米·秒,其余部分对布美他尼不敏感。如果内部透析液中同时存在氯离子、钾离子和ATP,在持续存在10⁻⁵ M哇巴因和10⁻⁷ M河豚毒素的情况下,10微摩尔布美他尼可抑制约5皮摩尔/平方厘米·秒的钠离子外流。然而,去除氯离子、钾离子或ATP会减少钠离子外流,使其对布美他尼不敏感。钾离子外流必须在电压钳制条件下进行研究,膜电位保持在 - 90 mV,因为钾离子外流的主要途径(延迟整流器)具有高度的电压敏感性。在这种电压钳制条件下,10微摩尔布美他尼可抑制1.8皮摩尔/平方厘米·秒的钾离子外流。所有这些结果都与紧密耦合的钠/钾/氯协同转运外流机制一致。此外,对顺式侧共离子和细胞内ATP的要求与先前描述的耦合钠/钾/氯内流过程完全相同。我们提出,同一个转运体介导内流和外流,因此证明了“可逆性”,这是离子梯度驱动转运过程的必要属性。

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