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首页> 外文期刊>Journal of Neurochemistry: Offical Journal of the International Society for Neurochemistry >A charybdotoxin-sensitive, Ca(2+)-activated K+ channel with inward rectifying properties in brain microvascular endothelial cells: properties and activation by endothelins.
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A charybdotoxin-sensitive, Ca(2+)-activated K+ channel with inward rectifying properties in brain microvascular endothelial cells: properties and activation by endothelins.

机译:Charybdotoxin敏感,Ca(2+)激活的K +通道在脑微血管内皮细胞中具有向内整流特性:内皮素的特性和激活。

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摘要

A charybdotoxin-sensitive, Ca(2+)-activated K+ channel was identified in cultured rat brain capillary endothelial cells by using conventional single-channel recording techniques and 86(Rb+)-influx and efflux experiments. Channel activity was dependent on the presence of Ca2+ on the cytosolic face of the membrane with a threshold concentration of 100 nM. It was inhibited by charybdotoxin (IC50 30 nM) and quinine (IC50 0.1 mM) but not by apamin. K(Ca) channels showed unusual inward rectifying properties under asymmetrical ionic conditions. They were activated by endothelin-1 (EC50 0.7 nM) and endothelin-3 (EC50 7-10 nM). The actions of endothelins were prevented by BQ-123 (Ki = 8 nM) in a competitive fashion, hence suggesting the involvement of an ETA-receptor subtype. The channel activity was unaffected by cyclic AMP- or cyclic GMP-elevating agents. The possible role of the intermediate conductance, Ca(2+)-activated K+ channels for mediating K+ movements across the blood-brain barrier is discussed.
机译:通过使用常规单通道记录技术和86(Rb +)流入和流出实验,在培养的大鼠脑毛细血管内皮细胞中鉴定出一种对Charybdotoxin敏感的Ca(2+)激活的K +通道。通道活性取决于膜胞质表面上Ca2 +的存在,阈值浓度为100 nM。它被甲藻毒素(IC50 30 nM)和奎宁(IC50 0.1 mM)抑制,但被阿帕明抑制。 K(Ca)通道在不对称离子条件下显示出异常的向内整流特性。它们被内皮素-1(EC50 0.7 nM)和内皮素3(EC50 7-10 nM)激活。 BQ-123(Ki = 8 nM)以竞争性方式阻止了内皮素的作用,因此暗示了ETA受体亚型的参与。通道活性不受环状AMP或环状GMP升高剂的影响。讨论了中间电导,Ca(2+)激活的K +通道介导跨血脑屏障的K +运动的可能作用。

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