去氧肾上腺素对大鼠小肠系膜动脉中内皮源性血管舒张因子释放的间接影响。
An indirect influence of phenylephrine on the release of endothelium-derived vasodilators in rat small mesenteric artery.
作者信息
Dora K A, Hinton J M, Walker S D, Garland C J
机构信息
Cardiovascular Research Laboratories and Department of Pharmacology, University of Bristol, University Walk, Bristol BS8 1TD, UK.
出版信息
Br J Pharmacol. 2000 Jan;129(2):381-7. doi: 10.1038/sj.bjp.0703052.
Abstract
- The possibility that stimulation of smooth muscle alpha(1)-adrenoceptors modulates contraction via the endothelium was examined in rat small mesenteric arteries. 2. N(omega)-nitro-L-arginine methyl ester, (L-NAME, 100 microM to inhibit NO synthase) increased contraction to single concentrations of phenylephrine (1 - 3 microM) by approximately 2 fold (from a control level of 14.2+/-3.0 to 34. 1+/-4.2% of the maximum contraction of the artery, n=20). The action of L-NAME was abolished by disrupting the endothelium. 3. The subsequent addition of apamin (to inhibit small conductance Ca(2+)-activated K(+) channels, 50 nM) further augmented phenylephrine contractions, in an endothelium-dependent manner, to more than 3 fold above control (50.4+/-5.3% of the maximum contraction, n=11). 4.Charybdotoxin (non-selective inhibitor of large conductance Ca(2+)-activated K(+) channels, BK(Ca), 50 nM) plus L-NAME augmented the level of phenylephrine contraction to 4 - 5-fold above control (64.1+/-3.1%, n=5), but this effect was independent of the endothelium. The potentiation of contraction by charybdotoxin could be mimicked with the selective BK(Ca) inhibitor, iberiotoxin,. 5. Apamin together with L-NAME and charybdotoxin further significantly increased the phenylephrine contraction by 5 - 6-fold, to 79.9+/-3.5% of the maximum contraction of the artery (n=13). 6. Phenylephrine failed directly to increase the intracellular Ca(2+) concentration in endothelial cells freshly isolated from the small mesenteric artery. 7. Stimulation of smooth muscle alpha(1)-adrenoceptors in the mesenteric artery induces contraction that is markedly suppressed by the endothelium. The attenuation of contraction appears to reflect both the release of NO from the endothelium and the efflux of K(+) from both endothelial and smooth muscle cells. This suggests that the release of NO and endothelium-derived hyperpolarizing factor can be evoked indirectly by agents which act only on the smooth muscle cells.
摘要
- 在大鼠小肠系膜动脉中研究了刺激平滑肌α(1)-肾上腺素能受体是否通过内皮调节收缩。2. N(ω)-硝基-L-精氨酸甲酯(L-NAME,100微摩尔抑制一氧化氮合酶)使对单浓度去氧肾上腺素(1 - 3微摩尔)的收缩增加约2倍(从动脉最大收缩的对照水平14.2±3.0增加到34.1±4.2%,n = 20)。破坏内皮可消除L-NAME的作用。3. 随后加入蜂毒明肽(抑制小电导钙激活钾通道,50纳摩尔)以依赖内皮的方式进一步增强去氧肾上腺素收缩,比对照增加超过3倍(最大收缩的50.4±5.3%,n = 11)。4. 大电导钙激活钾通道(BK(Ca))的非选择性抑制剂蝎毒素(50纳摩尔)加L-NAME使去氧肾上腺素收缩水平比对照增加4 - 5倍(64.1±3.1%,n = 5),但此效应不依赖内皮。蝎毒素对收缩的增强作用可用选择性BK(Ca)抑制剂iberiotoxin模拟。5. 蜂毒明肽与L-NAME和蝎毒素一起进一步显著增加去氧肾上腺素收缩5 - 6倍,达到动脉最大收缩的79.9±3.5%(n = 13)。6. 去氧肾上腺素不能直接增加从小肠系膜动脉新鲜分离的内皮细胞内的钙浓度。7. 刺激肠系膜动脉中的平滑肌α(1)-肾上腺素能受体诱导收缩,该收缩明显受内皮抑制。收缩的减弱似乎反映了内皮释放一氧化氮以及内皮细胞和平滑肌细胞中钾离子外流。这表明一氧化氮和内皮衍生超极化因子的释放可由仅作用于平滑肌细胞的药物间接诱发。
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