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缺氧对绵羊离体冠状动脉环药理反应性的影响。

Effects of hypoxia on the pharmacological responsiveness of isolated coronary artery rings from the sheep.

作者信息

Kwan Y W, Wadsworth R M, Kane K A

机构信息

Department of Physiology and Pharmacology, University of Strathclyde, Glasgow.

出版信息

Br J Pharmacol. 1989 Apr;96(4):849-56. doi: 10.1111/j.1476-5381.1989.tb11894.x.

Abstract
  1. The effects of low oxygen tension on tone and on the responsiveness to contractile and relaxant agents were examined on circumflex coronary artery rings isolated from sheep. 2. When artery rings (2-2.5 mm o.d.) were set at their optimal resting tension, introduction of hypoxia (0% O2) caused a sustained contraction which was reversible on washing with oxygenated Krebs solution. In precontracted (40 mM KCl) arteries, hypoxia caused a similar response except that it was preceded by a transient relaxation. 3. The hypoxia-induced contraction was potentiated by the combination of phentolamine (1 microM) and propranolol (1 microM), markedly reduced by verapamil (10 microM) and either abolished or reduced by indomethacin (1 microM). Indomethacin itself caused a contraction. 4. Under hypoxic conditions, the contractile effects of U46619 (a stable thromboxane analogue) and 5-hydroxytryptamine (5-HT) and the vasodilator effects of noradrenaline, iloprost (a prostacyclin mimetic) and adenosine were markedly potentiated. In contrast, vasoconstriction to potassium or acetylcholine was depressed. 5. Changing the gases from 95% O2 to 12% O2 had no significant effect on the contractile effects of U46619. However, the maximum contractile effect of U46619 was significantly enhanced by changing the gases from 12% O2 to 0% O2. 6. Rings from a smaller branch (0.6-1.3 mm o.d.) of the circumflex coronary artery of the sheep, in the presence of hypoxia, exhibited qualitatively similar changes in the responsiveness to U46619, 5-HT and adenosine to those observed in the large artery. However, the effect of potassium was potentiated rather than depressed. 7. It is concluded that hypoxia-induced contraction may involve a modified release of cyclooxygenase products and be partly dependent upon the availability of extracellular calcium. 8. The change in the responsiveness of coronary arteries, under hypoxia, to both constrictor and dilator mediators may have clinical relevance to myocardial ischaemia and angina pectoris.
摘要
  1. 研究了低氧张力对从绵羊分离的冠状动脉环张力以及对收缩剂和舒张剂反应性的影响。2. 当动脉环(外径2 - 2.5毫米)设定在其最佳静息张力时,引入低氧(0% O₂)会引起持续收缩,用含氧的克雷布斯溶液冲洗后可逆转。在预收缩(40 mM KCl)的动脉中,低氧引起类似反应,但在此之前有短暂舒张。3. 低氧诱导的收缩被酚妥拉明(1 microM)和普萘洛尔(1 microM)联合增强,被维拉帕米(10 microM)显著减弱,被吲哚美辛(1 microM)消除或减弱。吲哚美辛本身会引起收缩。4. 在低氧条件下,U46619(一种稳定的血栓素类似物)和5 - 羟色胺(5 - HT)的收缩作用以及去甲肾上腺素、伊洛前列素(一种前列环素模拟物)和腺苷的血管舒张作用显著增强。相比之下,对钾或乙酰胆碱的血管收缩作用受到抑制。5. 将气体从95% O₂ 变为12% O₂ 对U46619的收缩作用无显著影响。然而,将气体从12% O₂ 变为0% O₂ 可显著增强U46619的最大收缩作用。6. 绵羊冠状动脉较小分支(外径0.6 - 1.3毫米)的环在低氧存在下,对U46619、5 - HT和腺苷的反应性变化在性质上与在大动脉中观察到的相似。然而,钾的作用增强而非受到抑制。7. 得出结论,低氧诱导的收缩可能涉及环氧化酶产物的改变释放,并且部分依赖于细胞外钙的可用性。8. 冠状动脉在低氧条件下对收缩剂和舒张剂介质反应性的变化可能与心肌缺血和心绞痛的临床情况相关。

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