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从气道平滑肌重构的大电导钾通道。

Large conducting potassium channel reconstituted from airway smooth muscle.

作者信息

Savaria D, Lanoue C, Cadieux A, Rousseau E

机构信息

Department of Physiology, Faculty of Medicine, University of Sherbrooke, Quebec, Canada.

出版信息

Am J Physiol. 1992 Mar;262(3 Pt 1):L327-36. doi: 10.1152/ajplung.1992.262.3.L327.

DOI:10.1152/ajplung.1992.262.3.L327
PMID:1372487
Abstract

Microsomal fractions were prepared from canine and bovine airway smooth muscle (ASM) by differential and gradient centrifugations. Surface membrane vesicles were characterized by binding assays and incorporated into planar lipid bilayers. Single-channel activities were recorded in symmetric or asymmetric K+ buffer systems and studied under voltage and Ca2+ clamp conditions. A large-conductance K(+)-selective channel (greater than 220 pS in 150 mM K+) displaying a high Ca2+, low Ba2+, and charybdotoxin (CTX) sensitivity was identified. Time analysis of single-channel recordings revealed a complex kinetic behavior compatible with the previous schemes proposed for Ca(2+)-activated K+ channels in a variety of biological surface membranes. We now report that the open probability of the channel at low Ca2+ concentration is enhanced on in vitro phosphorylation, which is mediated via an adenosine 3',5'-cyclic monophosphate-dependent protein kinase. In addition to this characterization at the molecular level, a second series of pharmacological experiments were designed to assess the putative role of this channel in ASM strips. Our results show that 50 nM CTX, a specific inhibitor of the large conducting Ca(2+)-dependent K+ channel, prevents norepinephrine transient relaxation on carbamylcholine-precontracted ASM strips. It was also shown that CTX reversed the steady-state relaxation induced by vasoactive intestinal peptide and partially antagonized further relaxation induced by cumulative doses of this potent bronchodilatator. Thus it is proposed that the Ca(2+)-activated K+ channels have a physiological role because they are indirectly activated on stimulation of various membrane receptors via intracellular mechanisms.

摘要

通过差速离心和梯度离心从犬和牛的气道平滑肌(ASM)中制备微粒体部分。通过结合测定对表面膜囊泡进行表征,并将其整合到平面脂质双分子层中。在对称或不对称的K +缓冲系统中记录单通道活性,并在电压和Ca2 +钳制条件下进行研究。鉴定出一种大电导K(+)选择性通道(在150 mM K +中大于220 pS),其对Ca2 +、低Ba2 +和蝎毒素(CTX)具有高敏感性。单通道记录的时间分析揭示了一种复杂的动力学行为,这与先前为各种生物表面膜中Ca(2+)激活的K +通道提出的方案相一致。我们现在报告,在低Ca2 +浓度下,该通道的开放概率在体外磷酸化时会增强,这是通过腺苷3',5'-环磷酸依赖性蛋白激酶介导的。除了在分子水平上的这种表征外,还设计了第二系列药理实验来评估该通道在ASM条带中的假定作用。我们的结果表明,50 nM CTX是大电导Ca(2+)依赖性K +通道的特异性抑制剂,可阻止去甲肾上腺素对氨甲酰胆碱预收缩的ASM条带的瞬时松弛作用。还表明,CTX可逆转血管活性肠肽诱导的稳态松弛,并部分拮抗该强效支气管扩张剂累积剂量诱导的进一步松弛。因此,有人提出Ca(2+)激活的K +通道具有生理作用,因为它们在通过细胞内机制刺激各种膜受体时被间接激活。

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Large conducting potassium channel reconstituted from airway smooth muscle.从气道平滑肌重构的大电导钾通道。
Am J Physiol. 1992 Mar;262(3 Pt 1):L327-36. doi: 10.1152/ajplung.1992.262.3.L327.
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