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Effect of intracerebroventricular and intravenous administration of nitric oxide donors on blood pressure and heart rate in anaesthetized rats.

机译:脑室内和静脉内一氧化氮供体对麻醉大鼠血压和心率的影响。

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摘要

1. The effects of nitric oxide (NO) releasing substances, sodium nitroprusside, 3-morpholino sydnonimine (SIN-1) and a novel oxatriazole derivative, GEA 3162, on blood pressure and heart rate were studied after peripheral or central administration in anaesthetized normotensive Wistar rats. 2. Given as cumulative intravenous injections, both nitroprusside and GEA 3162 (24-188 nmol kg-1) induced short-lasting and dose-dependent decreases in mean arterial pressure, while SIN-1 decreased blood pressure only slightly even after larger doses (94-3000 nmol kg-1). Heart rate increased concomitantly with the hypotensive effect of the NO-releasing substances. 3. Cumulative intracerebroventricular administration of GEA 3162 (24-188 nmol kg-1) induced a dose-dependent hypotension with slight but insignificant increases in heart rate. In contrast, intracerebroventricular nitroprusside induced little change in blood pressure, while a large dose of SIN-1 (3000 nmol kg-1, i.c.v.) slightly increased mean arterial pressure. However, intracerebroventricular nitroprusside and SIN-1 increased heart rate at doses that did not significantly affect blood pressure. 4. To determine whether the cardiovascular effects of GEA 3162 were attributable to an elevation of cyclic GMP levels, pretreatments with methylene blue, a putative guanylate cyclase inhibitor, were performed. This substance failed to attenuate the cardiovascular effects of peripherally or centrally administered GEA 3162, suggesting that the effects were independent of guanylate cyclase. 5. In conclusion, the centrally administered NO-donor, GEA 3162, induced a dose-dependent. hypotensive response without significant changes in heart rate. Furthermore, intracerebroventricular injections of nitroprusside and SIN-1 increased heart rate without affecting blood pressure. These results suggest that NO released by these drugs may affect central mechanisms involved in cardiovascular regulation independently of cyclic GMP.
机译:1.在麻醉或降压的情况下,经外周或中枢给药后,研究了释放一氧化氮(NO)的物质硝普钠,3-吗啉代亚砜亚胺(SIN-1)和新型草三唑衍生物GEA 3162对血压和心率的影响。 Wistar大鼠。 2.以累积静脉注射的形式,硝普钠和GEA 3162(24-188 nmol kg-1)均会引起持续性且剂量依赖性的平均动脉压降低,而SIN-1甚至在大剂量给药后也仅略微降低了血压( 94-3000 nmol kg-1)。心率随NO释放物质的降压作用而增加。 3.累积性脑室内给药GEA 3162(24-188 nmol kg-1)引起剂量依赖性低血压,心率略有升高,但微不足道。相反,脑室内硝普钠诱导的血压变化很小,而大剂量的SIN-1(3000 nmol kg-1,i.c.v.)则使平均动脉压略有增加。然而,脑室内硝普钠和SIN-1在不显着影响血压的剂量下增加了心率。 4.为了确定GEA 3162的心血管作用是否归因于循环GMP水平的升高,进行了亚甲基蓝(一种假定的鸟苷酸环化酶抑制剂)的预处理。该物质未能减弱外围或集中给药的GEA 3162的心血管作用,表明这种作用与鸟苷酸环化酶无关。 5.总之,集中管理的NO供体GEA 3162诱导了剂量依赖性。降压反应,心率无明显变化。此外,脑室内注射硝普钠和SIN-1可增加心率,而不会影响血压。这些结果表明,这些药物释放的NO可能独立于循环GMP而影响参与心血管调节的中枢机制。

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