Azulene - 1 - carboxamidine衍生物N1, N1 -二甲基- N2 - (2 - pyridylmethyl) - 5 -异丙基- 3,8 -二甲基- 1 - carboxamidine (HNS - 32)对猪冠状动脉的松弛作用

Yoshio Tanaka Makoto Kamibayashi, F. Yamaki, M. Saitoh, T. Nakazawa, Hikaru Tanaka, K. Noguchi, K. Hashimoto, K. Shigenobu
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引用次数: 23

摘要

HNS-32 (n1n1 -二甲基- n2 -(2-吡啶基甲基)-5-异丙基-3,8-二甲基苄基-1-羧基脒)(CAS 186086-10-2)是一种新合成的分子内具有azulene结构的化合物。用药理学方法研究了HNS-32对离体猪冠状动脉的舒张作用。将HNS-32的作用与钙离子通道阻滞剂地尔硫卓进行比较。HNS-32以浓度依赖的方式抑制高KCl、前列腺素F2α、血栓素A2模拟物(U46619)和内皮素-1引起的持续收缩。HNS-32抑制这些收缩的效力比地尔硫卓低5- 40倍。HNS-32还能减少乙酰胆碱、组胺和5-羟色胺引起的期相收缩。过量Ca2+的加入仅抵消了hns -32诱导的高kcl诱导的收缩抑制约10%,而它恢复了地尔硫卓诱导的抑制约50%。HNS-32对phorbol酯(phorbol 12,13-二丁酸酯)的收缩反应抑制约为40%。HNS-32可预防多种痉挛原引起的冠状动脉收缩。虽然对l型Ca2+通道和蛋白激酶C的抑制可能是HNS-32作用的部分原因,但HNS-32对收缩系统的一些直接作用似乎参与了冠状动脉舒张。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Relaxant Action of Azulene‐1‐carboxamidine Derivative N1, N1‐dimethyl‐N2‐(2‐pyridylmethyl)‐5‐isopropyl‐3,8‐dimethylazulene‐1‐carboxamidine (HNS‐32) in Pig Coronary Artery
HNS-32 (N1N1-dimethyl-N2-(2-pyridylmethyl)-5-isopropyl-3,8-dimethylazulene-1-carbox-amidine) (CAS 186086-10-2) is a newly synthesized compound with an azulene structure within the molecule. The coronary relaxant action of HNS-32 was investigated pharmaco-mechanically on isolated pig coronary artery. The effects of HNS-32 were compared with diltiazem, a Ca2+-channel blocker. HNS-32 inhibited sustained contractions evoked by high KCl, prostaglandin F2α, a thromboxane A2 mimetic (U46619) and endothelin-1 in a concentration-dependent manner. The potency of HNS-32 to inhibit these contractions was 5- to 40-times lower than diltiazem. HNS-32 also diminished phasic contractions induced by acetylcholine, histamine and 5-hydroxytryptamine. Addition of excess Ca2+ counteracted HNS-32-induced inhibition of high KCl-induced contraction only by approximately 10% whereas it restored diltiazem-induced inhibition by about 50%. Suppression of the contractile response to a phorbol ester (phorbol 12,13-dibutyrate) by HNS-32 was approximately 40%. HNS-32 prevents coronary contractions produced by a wide variety of spasmogens. Although inhibitions of L-type Ca2+ channels and protein kinase C may be partly responsible for HNS-32 action, some direct action on the contractile systems seems to be involved in the coronary relaxation by HNS-32.
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