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各种钙离子通道拮抗剂对大鼠吗啡镇痛、耐受性和依赖性以及血压的影响。

Effects of various Ca2+ channel antagonists on morphine analgesia, tolerance and dependence, and on blood pressure in the rat.

作者信息

Michaluk J, Karolewicz B, Antkiewicz-Michaluk L, Vetulani J

机构信息

Institute of Pharmacology, Polish Academy of Sciences, Krakow.

出版信息

Eur J Pharmacol. 1998 Jul 10;352(2-3):189-97. doi: 10.1016/s0014-2999(98)00373-2.

Abstract

Following the finding that nifedipine enhances morphine analgesia and prevents the development of dependence, we have now compared the effect of nifedipine with these of other L-type Ca2+ channel antagonists, nimodipine (a dihydropyridine) and verapamil (a phenylethylalkylamine). Male Wistar rats received the antagonist 20 min before each injection of morphine. Analgesia was measured in a hot-plate test, and the development of dependence was assessed in the naloxone precipitation test after 13 days of morphine (20-30 mg/kg i.p.) administration. L-type Ca2+ channels were assayed in the cerebral cortex as [3H]nitrendipine binding sites. Blood pressure was monitored from the tail by a non-invasive method. We found that all three Ca2+ antagonists enhanced the analgesia, and prevented development of the naloxone-precipitated withdrawal syndrome, although they differed in their efficacy. Nifedipine and verapamil effectively blocked the development of tolerance. While chronic morphine up-regulated L-type Ca2+ channels, co-administration of the antagonists completely prevented this effect. The effects of Ca2+ channel antagonists cannot be ascribed to their potential circulatory effects as, at the dose used, none affected significantly the arterial blood pressure.

摘要

在发现硝苯地平可增强吗啡镇痛作用并预防依赖性形成后,我们现在比较了硝苯地平与其他L型钙通道拮抗剂尼莫地平(一种二氢吡啶类)和维拉帕米(一种苯乙烷基胺类)的作用。雄性Wistar大鼠在每次注射吗啡前20分钟接受拮抗剂。通过热板试验测量镇痛作用,并在给予吗啡(20 - 30mg/kg腹腔注射)13天后,通过纳洛酮催瘾试验评估依赖性的形成。以[3H]尼群地平结合位点测定大脑皮层中的L型钙通道。采用无创方法从尾部监测血压。我们发现,尽管三种钙拮抗剂的效力有所不同,但它们均增强了镇痛作用,并预防了纳洛酮诱发的戒断综合征的出现。硝苯地平和维拉帕米有效阻断了耐受性的形成。慢性吗啡使L型钙通道上调,而同时给予拮抗剂则完全预防了这种作用。钙通道拮抗剂的作用不能归因于其潜在的循环系统作用,因为在所使用的剂量下,它们均未显著影响动脉血压。

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