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脑室内注射组胺对麻醉大鼠心血管系统的影响。

The cardiovascular effects of intraventricularly administered histamine in the anaesthetised rat.

作者信息

Finch L, Hicks P E

出版信息

Naunyn Schmiedebergs Arch Pharmacol. 1976 May;293(2):151-7. doi: 10.1007/BF00499220.

Abstract

In urethane-anaestetised rats intraventricular (i.c.v.) injections of histamine (0.1-10.0mug) elicited dose-related rises in both the resting blood pressure and heart rate. These cardiovascular effects of histamine were antagonised in a dose-dependent manner by i.c.v. pretreatments with the histamine H1-receptor antagonists mepyramine (10, 50 and 100 mug) and diphenylpyraline (100 and 200mug). Pretreatment with the histamine H2-receptor antagonist metiamide (100 and 200 mug i.c.v.) failed to modify either of the responses. A dose-related antagonism of the hypertensive response to histamine i.c.v. was elicited by phentolamine (100 and 200 mug i.c.v.) but the positive chronotropic effect was not modified by this pretreatment. The cardiovascular responses to histamine i.c.v. were abolished by mecamylamine (5.0 mg/kg i.v.) and greatly reduced by 6-hydroxydopamine (3 X 250 mug i.c.v.), but only the tachycardia was significantly modified by atropine (100 mug i.c.v.) and propranolol (1 mg/kg i.v.). Propranolol (100 mug i.c.v.), bilateral vagotomy, or acute bilateral adrenal demedullation failed to modify the cardiovascular responses to histamine i.c.v. The results suggest that histamine is able to modify the resting blood pressure and heart rate by independent central modes of action, which involve central adrenergic and cholinergic mechanisms.

摘要

在氨基甲酸乙酯麻醉的大鼠中,脑室内(i.c.v.)注射组胺(0.1 - 10.0微克)会引起静息血压和心率呈剂量相关的升高。组胺的这些心血管效应可被脑室内预先给予组胺H1受体拮抗剂美吡拉敏(10、50和100微克)和二苯拉林(100和200微克)以剂量依赖的方式拮抗。预先给予组胺H2受体拮抗剂甲硫米特(脑室内注射100和200微克)未能改变任何一种反应。酚妥拉明(脑室内注射100和200微克)可引起对脑室内注射组胺所致高血压反应的剂量相关拮抗作用,但这种预处理并未改变正性变时效应。脑室内注射组胺引起的心血管反应可被美加明(静脉注射5.0毫克/千克)消除,并被6 - 羟基多巴胺(脑室内注射3×250微克)大大降低,但只有心动过速被阿托品(脑室内注射100微克)和普萘洛尔(静脉注射1毫克/千克)显著改变。普萘洛尔(脑室内注射100微克)、双侧迷走神经切断术或急性双侧肾上腺髓质剥除术均未能改变对脑室内注射组胺的心血管反应。结果表明,组胺能够通过独立的中枢作用模式改变静息血压和心率,这些模式涉及中枢肾上腺素能和胆碱能机制。

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