人 big-内皮素-1、2(1-38)和 3 在氯胺酮/甲苯噻嗪麻醉的豚鼠体内的不同升压和支气管收缩特性
Different pressor and bronchoconstrictor properties of human big-endothelin-1, 2 (1-38) and 3 in ketamine/xylazine-anaesthetized guinea-pigs.
作者信息
Gratton J P, Rae G A, Claing A, Télémaque S, D'Orléans-Juste P
机构信息
Department of Pharmacology, Medical School, Université de Sherbrooke, Québec, Canada.
出版信息
Br J Pharmacol. 1995 Feb;114(3):720-6. doi: 10.1111/j.1476-5381.1995.tb17198.x.
Abstract
- In the present study, the precursors of endothelin-1, endothelin-2 and endothelin-3 were tested for their pressor and bronchoconstrictor properties in the anaesthetized guinea-pig. In addition, the effects of big-endothelin-1 and endothelin-1 were assessed under urethane or ketamine/xylazine anaesthesia. 2. When compared to ketamine/xylazine, urethane markedly depressed the pressor and bronchoconstrictor properties of endothelin-1 and big-endothelin-1. 3. Under ketamine/xylazine anaesthesia, the three endothelins induced a biphasic increase of mean arterial blood pressure. In contrast, big-endothelin-1, as well as big-endothelin-2 (1-38), induced only sustained increase in blood pressure whereas big-endothelin-3 was inactive at doses up to 25 nmol kg-1. 4. Big-endothelin-1, but not big-endothelin-2, induced a significant increase in airway resistance. Yet, endothelin-1, endothelin-2 and endothelin-3 were equipotent as bronchoconstrictor agents. 5. Big-endothelin-1, endothelin-1 and endothelin-2, but not big-endothelin-2, triggered a marked release of prostacyclin and thromboxane A2 from the guinea-pig perfused lung. 6. Our results suggest the presence of a phosphoramidon-sensitive endothelin-converting enzyme (ECE) which is responsible for the conversion of big-endothelin-1 and big-endothelin-2 to their active moieties, endothelin-1 and 2. However, the lack of bronchoconstrictor and eicosanoid-releasing properties of big-endothelin-2, as opposed to endothelin-2 or big-endothelin-1, suggests the presence of two distinct phosphoramidon-sensitive ECEs in the guinea-pig. The ECE responsible for the systemic conversion of big-endothelins possesses the same affinity for big-endothelin-l and 2 but not big-endothelin-3. In contrast, in the pulmonary vasculature is localized in the vicinity of the sites responsible for eicosanoid release, an ECE which converts more readily big-endothelin-1 than big-endothelin-2.
摘要
- 在本研究中,检测了内皮素 -1、内皮素 -2和内皮素 -3的前体在麻醉豚鼠中的升压和支气管收缩特性。此外,还评估了大内皮素 -1和内皮素 -1在氨基甲酸乙酯或氯胺酮/赛拉嗪麻醉下的作用。2. 与氯胺酮/赛拉嗪相比,氨基甲酸乙酯显著降低了内皮素 -1和大内皮素 -1的升压和支气管收缩特性。3. 在氯胺酮/赛拉嗪麻醉下,三种内皮素引起平均动脉血压双相升高。相比之下,大内皮素 -1以及大内皮素 -2(1 - 38)仅引起血压持续升高,而大内皮素 -3在剂量高达25 nmol·kg⁻¹时无活性。4. 大内皮素 -1而非大内皮素 -2引起气道阻力显著增加。然而,内皮素 -1、内皮素 -2和内皮素 -3作为支气管收缩剂具有同等效力。5. 大内皮素 -1、内皮素 -1和内皮素 -2而非大内皮素 -2引发了豚鼠灌注肺中前列环素和血栓素A2的显著释放。6. 我们的结果表明存在一种对磷酰胺敏感的内皮素转换酶(ECE),它负责将大内皮素 -1和大内皮素 -2转化为它们的活性部分,即内皮素 -1和内皮素 -2。然而,与内皮素 -2或大内皮素 -1不同,大内皮素 -2缺乏支气管收缩和类花生酸释放特性,这表明豚鼠中存在两种不同的对磷酰胺敏感的ECE。负责大内皮素全身转化的ECE对大内皮素 -1和大内皮素 -2具有相同的亲和力,但对大内皮素 -3没有。相比之下,在肺血管系统中,在负责类花生酸释放的部位附近定位有一种ECE,它将大内皮素 -1转化为内皮素 -1比将大内皮素 -2转化为内皮素 -2更容易。
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