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两种不同的氧传感器调节鲫鱼红细胞中对氧敏感的钾离子转运。

Two different oxygen sensors regulate oxygen-sensitive K+ transport in crucian carp red blood cells.

作者信息

Berenbrink Michael, Völkel Susanne, Koldkjaer Pia, Heisler Norbert, Nikinmaa Mikko

机构信息

School of Biological Sciences, The University of Liverpool, Biosciences Building, Crown Street, Liverpool L69 7ZB, UK.

出版信息

J Physiol. 2006 Aug 15;575(Pt 1):37-48. doi: 10.1113/jphysiol.2006.112680. Epub 2006 Jun 8.

Abstract

The O2 dependence of ouabain-independent K+ transport mechanisms has been studied by unidirectional Rb+ flux analysis in crucian carp red blood cells (RBCs). The following observations suggest that O2 activates K+-Cl- cotransport (KCC) and deactivates Na+-K+-2Cl- cotransport (NKCC) in these cells via separate O2 sensors that differ in their O2 affinity. When O2 tension (PO2) at physiological pH 7.9 was increased from 0 to 1, 4, 21 or 100 kPa, K+ (Rb+) influx was increasingly inhibited, and at 100 kPa amounted to about 30% of the value at 0 kPa. This influx was almost completely Cl- dependent at high and low PO2, as shown by substituting Cl- with nitrate or methanesulphonate. K+ (Rb+) efflux showed a similar PO2 dependence as K+ (Rb+) influx, but was about 4-5 times higher over the whole PO2 range. The combined net free energy of transmembrane ion gradients favoured net efflux of ions for both KCC and NKCC mechanisms. The KCC inhibitor dihydroindenyloxyalkanoic acid (DIOA, 0.1 mM) abolished Cl- -dependent K+ (Rb+) influx at a PO2 of 100 kPa, but was only partially effective at low PO2 (0-1 kPa). At PO2 values between 0 and 4 kPa, K+ (Rb+) influx was further unaffected by variations in pH between 8.4 and 6.9, whereas the flux at 21 and 100 kPa was strongly reduced by pH values below 8.4. At pH 8.4, where K+ (Rb+) influx was maximal at high and low PO2, titration of K+ (Rb+) influx with the NKCC inhibitor bumetanide (1, 10 and 100 microM) revealed a highly bumetanide-sensitive K+ (Rb+) flux pathway at low PO2, and a relative bumetanide-insensitive pathway at high PO2. The bumetanide-sensitive K+ (Rb+) influx pathway was activated by decreasing PO2, with a PO2 for half-maximal activation (P50) not significantly different from the P50 for haemoglobin O2 binding. The bumetanide-insensitive K+ (Rb+) influx pathway was activated by increasing PO2 with a P50 significantly higher than for haemoglobin O2 binding. These results are relevant for the pathologically altered O2 sensitivity of RBC ion transport in certain human haemoglobinopathies.

摘要

通过对鲫鱼红细胞(RBC)进行单向铷离子通量分析,研究了哇巴因非依赖性钾离子转运机制对氧气的依赖性。以下观察结果表明,在这些细胞中,氧气通过具有不同氧气亲和力的独立氧气传感器激活钾离子-氯离子协同转运(KCC)并使钠离子-钾离子-2氯离子协同转运(NKCC)失活。当生理pH值7.9时的氧气张力(PO2)从0增加到1、4、21或100 kPa时,钾离子(铷离子)内流受到越来越强的抑制,在100 kPa时约为0 kPa时的30%。如用硝酸盐或甲磺酸盐替代氯离子所示,在高和低PO2时,这种内流几乎完全依赖于氯离子。钾离子(铷离子)外流与钾离子(铷离子)内流表现出相似的PO2依赖性,但在整个PO2范围内高出约4-5倍。跨膜离子梯度的总自由能有利于KCC和NKCC机制的离子净外流。KCC抑制剂二氢茚氧基链烷酸(DIOA,0.1 mM)在PO2为100 kPa时消除了氯离子依赖性钾离子(铷离子)内流,但在低PO2(0-1 kPa)时仅部分有效。在PO2值为0至4 kPa之间,钾离子(铷离子)内流不受pH值在8.4和6.9之间变化的影响,而在21和100 kPa时的通量在pH值低于8.4时显著降低。在pH 8.4时,高和低PO2下钾离子(铷离子)内流最大,用NKCC抑制剂布美他尼(1、10和100 microM)滴定钾离子(铷离子)内流显示,在低PO2时有一条对布美他尼高度敏感的钾离子(铷离子)通量途径,在高PO2时有一条相对对布美他尼不敏感的途径。布美他尼敏感的钾离子(铷离子)内流途径通过降低PO2激活,其半数最大激活的PO2(P50)与血红蛋白氧气结合的P50无显著差异。布美他尼不敏感的钾离子(铷离子)内流途径通过增加PO2激活,其P50显著高于血红蛋白氧气结合的P50。这些结果与某些人类血红蛋白病中红细胞离子转运的病理改变的氧气敏感性相关。

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