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组胺诱导离体猴和犬冠状动脉舒张的机制。

Mechanisms of histamine-induced relaxation in isolated monkey and dog coronary arteries.

作者信息

Toda N

出版信息

J Pharmacol Exp Ther. 1986 Nov;239(2):529-35.

PMID:3772808
Abstract

Relaxations induced by histamine in helical strips of monkey coronary arteries were attenuated either by chlorpheniramine or cimetidine; the H1 antagonist suppressed the fast component of relaxation, whereas the H2 antagonist reduced the slow component. Combined treatment with these antagonists abolished the amine-induced relaxation. The relaxation was not influenced by indomethacin; however, the fast component of relaxation was inhibited by 5, 8, 11, 14-eicosatetraynoic acid, AA861, a lipoxygenase inhibitor, and methylene blue. In the arteries treated with methylene blue, relaxations were abolished by cimetidine. Removal of the endothelium reduced the relaxation markedly or reversed the relaxation to a contraction; chlorpheniramine reversed the contraction to a relaxation. In dog coronary arterial strips, histamine-induced relaxations were not attenuated by removal of the endothelium. Cimetidine shifted the dose-response curve for histamine to the right, but chlorpheniramine did not alter the response. Indomethacin, AA861 and methylene blue failed to inhibit the relaxation. The response of monkey coronary arteries to histamine appears to be a sum of the slight, persistent contraction, the transient relaxation and the slowly developing relaxation. The transient relaxation may be mediated by H1 receptors in the endothelium, the activation of which yields relaxing factor, resulting in an increase of cellular cyclic GMP in smooth muscle. The contraction and the slow relaxation appear to be associated with H1 and H2 receptors, respectively, in smooth muscle cells. Dog coronary arterial relaxations induced by histamine may be mediated exclusively by H2 receptors in muscle cell membrane.

摘要

组胺引起的猴冠状动脉螺旋条带舒张作用,可被氯苯那敏或西咪替丁减弱;H1拮抗剂抑制舒张的快速成分,而H2拮抗剂则减少舒张的缓慢成分。这两种拮抗剂联合处理可消除胺诱导的舒张。吲哚美辛不影响该舒张;然而,5,8,11,14-二十碳四烯酸、脂氧合酶抑制剂AA861和亚甲蓝可抑制舒张的快速成分。在用亚甲蓝处理的动脉中,西咪替丁可消除舒张。去除内皮可使舒张明显减弱或使舒张逆转至收缩;氯苯那敏可使收缩逆转至舒张。在犬冠状动脉条带中,去除内皮不会减弱组胺诱导的舒张。西咪替丁使组胺的剂量-反应曲线右移,但氯苯那敏不改变反应。吲哚美辛、AA861和亚甲蓝均未能抑制舒张。猴冠状动脉对组胺的反应似乎是轻微的持续性收缩、短暂舒张和缓慢发展的舒张的总和。短暂舒张可能由内皮中的H1受体介导,其激活产生舒张因子,导致平滑肌细胞内细胞环鸟苷酸增加。收缩和缓慢舒张似乎分别与平滑肌细胞中的H1和H2受体有关。组胺诱导的犬冠状动脉舒张可能仅由肌细胞膜中的H2受体介导。

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