Tamura T, Taniguchi T, Aoki M, Waki I
Central Research Laboratories, Nihon Iyakuhin Kogyo Co., Ltd., Toyama, Japan.
Nihon Yakurigaku Zasshi. 1990 Apr;95(4):167-75. doi: 10.1254/fpj.95.4_167.
Cerebral protective effect of eptazocine, a mu-antagonist-kappa-agonist, was investigated using mice subjected to hypoxia-anoxia. Eptazocine (1 to 10 mg/kg) prolonged the survival time of mice subjected to KCN (3 mg/kg, i.v.) injection in a dose-dependent manner, and this effect was completely inhibited by naloxone (5 mg/kg). EKC, U50,488H, opioid kappa-agonists, also had such an effect, but were weaker than eptazocine. In mice exposed to hypobaric hypoxia (190 mmHg), eptazocine (3, 10 mg/kg) and EKC (10 mg/kg) prolonged the survival time, but morphine (5 mg/kg) and pentazocine (10 mg/kg) shortened the time. The eptazocine effect was attenuated by either naloxone (5 mg/kg) or atropine (0.5 mg/kg), different from what was seen in the case of physostigmine and diazepam, and the combination of eptazocine (1 mg/kg) and physostigmine (0.075 mg/kg) had a potentiating effect. MR-2266, a selective kappa-receptor antagonist, inhibited the eptazocine effect more potently than naloxone. These results suggest that eptazocine elicited its cerebral protective effect via its binding with opioid kappa-receptors and probably an activation of the central cholinergic system.
使用缺氧-缺血小鼠研究了μ-拮抗剂-κ-激动剂依托唑啉的脑保护作用。依托唑啉(1至10毫克/千克)以剂量依赖性方式延长了接受静脉注射氰化钾(3毫克/千克)的小鼠的存活时间,且该作用被纳洛酮(5毫克/千克)完全抑制。阿片类κ-激动剂EKC、U50,488H也有这种作用,但比依托唑啉弱。在低压缺氧(190毫米汞柱)的小鼠中,依托唑啉(3、10毫克/千克)和EKC(10毫克/千克)延长了存活时间,但吗啡(5毫克/千克)和喷他佐辛(10毫克/千克)缩短了时间。依托唑啉的作用被纳洛酮(5毫克/千克)或阿托品(0.5毫克/千克)减弱,这与毒扁豆碱和地西泮的情况不同,且依托唑啉(1毫克/千克)和毒扁豆碱(0.075毫克/千克)的组合具有增强作用。选择性κ-受体拮抗剂MR-2266比纳洛酮更有效地抑制了依托唑啉的作用。这些结果表明,依托唑啉通过与阿片类κ-受体结合并可能激活中枢胆碱能系统发挥其脑保护作用。
