Daniel E E, Jury J, Salapatek A M, Bowes T, Lam A, Thomas S, Ramnarain M, Nguyen V, Mistry V
Department of Medicine, McMaster University, Hamilton, Ontario,
J Pharmacol Exp Ther. 2000 Jul;294(1):270-9.
In canine lower esophageal sphincter, myogenic constitutive nitric-oxide (NO) synthase (NOS) in plasma membrane limits tone by opening large conductance Ca(2+)-dependent K(+) channels (BK(Ca) channels) and hyperpolarizing the membrane. We examined whether K(V) channels were involved and whether NO from enteric nerves and from NO donors used the same mechanisms. With nerves inactive, 100 nM iberiotoxin, like N-nitro-L-arginine (L-NOARG), increased tone but less. 4-Aminopyridine (4-AP) at 5 mM behaved similarly. Tetraethyl ammonium (TEA) at 20 mM equaled the effect of L-NOARG and occluded any tone increase from any combination of these agents. More than iberiotoxin or 4-AP, TEA decreased relaxations in response to sodium nitroprusside (SNP) or 3-morpholino-sydnonimine (Sin-1) by approximately 50%. In whole-cell patch-clamp recordings, TEA and 4-AP reduced outward K(+) currents additively by >90% at depolarization of +90 mV. Thus, K(+) channels in addition to BK(Ca) channels are opened by myogenic NO, and exogenous NO had relaxing effects both related and unrelated to K(+) channel openings. TEA (20 mM) increased tone but did not inhibit relaxations to electrical field stimulation (EFS) of enteric nerves. 4-AP relaxed tone, an effect that was abolished and reversed by L-NOARG. 4-AP apparently released NO and acetylcholine from nerves. The putative Cl(-) channel blocker niflumic acid (NFA; 30-100 microM) dose dependently reduced tone, but tone, restored by 10(-6) M carbachol or 20 mM TEA, was still relaxed by EFS and by SNP. 4,4'-Diisothiocyanatostilbene-2, 2'-disulfonic acid (DIDS) at 500 to 1000 microM did not inhibit relaxation to EFS or SNP. The addition of TEA (20 mM) to DIDS (1000 microM) induced tonic and phasic activity and markedly inhibited relaxations to EFS. DIDS plus TEA reduced the relaxations to SNP like TEA alone. Reduction in extracellular ¿Cl(-) by isethionate substitution reduced tone but did not reduce relaxations when tone was restored. The combination of reduced extracellular ¿Cl(-) and TEA did not abolish relaxation to EFS until DIDS was added. Thus, multiple K(+) channels are opened by myogenic NO, and openings of these channels, as well as DIDS-sensitive, undefined mechanisms, are induced when NO is released from nerves or SNP.
在犬类下食管括约肌中,质膜中的肌源性组成型一氧化氮(NO)合酶(NOS)通过打开大电导钙依赖性钾通道(BK(Ca)通道)并使膜超极化来限制张力。我们研究了钾离子通道(K(V)通道)是否参与其中,以及来自肠神经和NO供体的NO是否使用相同的机制。在神经无活性的情况下,100 nM的iberiotoxin与N-硝基-L-精氨酸(L-NOARG)一样,可增加张力,但增加幅度较小。5 mM的4-氨基吡啶(4-AP)表现类似。20 mM的四乙铵(TEA)产生的效果与L-NOARG相当,并且消除了这些药物任何组合引起的张力增加。与iberiotoxin或4-AP相比,TEA使硝普钠(SNP)或3-吗啉代-西多奈明(Sin-1)引起的松弛反应降低了约50%。在全细胞膜片钳记录中,在+90 mV去极化时,TEA和4-AP相加使外向钾电流减少>90%。因此,除了BK(Ca)通道外,肌源性NO还可打开钾离子通道,外源性NO的松弛作用与钾离子通道开放有关和无关。20 mM的TEA增加了张力,但不抑制对肠神经电场刺激(EFS)的松弛反应。4-AP使张力松弛,L-NOARG可消除并逆转这种作用。4-AP显然从神经中释放了NO和乙酰胆碱。假定的氯离子通道阻滞剂氟尼酸(NFA;30 - 100 microM)剂量依赖性地降低了张力,但由10^(-6) M卡巴胆碱或20 mM TEA恢复的张力仍可被EFS和SNP松弛。500至1000 microM的4,4'-二异硫氰酸根合芪-2,2'-二磺酸(DIDS)不抑制对EFS或SNP的松弛反应。将20 mM的TEA添加到1000 microM的DIDS中会诱导强直和相位活动,并显著抑制对EFS的松弛反应。DIDS加TEA使对SNP的松弛反应降低程度与单独使用TEA时相同。用羟乙基磺酸替代降低细胞外氯离子浓度可降低张力,但当张力恢复时不降低松弛反应。细胞外氯离子浓度降低与TEA的组合直到添加DIDS才消除对EFS的松弛反应。因此,肌源性NO可打开多个钾离子通道,当NO从神经或SNP释放时,这些通道的开放以及DIDS敏感的、未明确的机制会被诱导。
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