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首页> 外文期刊>Scandinavian journal of gastroenterology. >Hemodynamic effects of substance P and its receptor antagonist RP67580 in anesthetized rats with carbon tetrachloride-induced cirrhosis
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Hemodynamic effects of substance P and its receptor antagonist RP67580 in anesthetized rats with carbon tetrachloride-induced cirrhosis

机译:P物质及其受体拮抗剂RP67580对麻醉的四氯化碳肝硬化大鼠的血流动力学影响

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摘要

Objective. Substance P (SP) is a vasodilator that may contribute to systemic and splanchnic vasodilatation in cirrhosis. The aim of this study was to determine the effects of SP (dose -13 pg/kg) and its specific inhibitor, RP67580 (dose - 300 mug/kg) on mean arterial pressure (MAP) and portal pressure (PP) in cirrhotic rats and controls. Material and methods. MAP and PP were measured before and after administering SP and RP67580. Additionally, a small group of cirrhotic rats were pretreated with L-NAME to block the effects of nitric oxide (NO) before measurements. Results. SP produced transient systemic hypotension in both groups. SP caused a significant increase in PP in cirrhotic rats and a decrease in PP in controls. RP67580 reduced the hypotensive effect of SP, but not completely. RP67580 decreased PP in the cirrhotic group but not in controls. In cirrhotic rats pretreated with L-NAME, SP administration caused a significant decrease in MAP but no significant change in PP. Conclusions. Exogenous SP increases PP and decreases MAP in cirrhotic rats. RP687580 decreases PP and reduces SP-induced hypotension in cirrhotic rats. NO blockade abolishes the effect of SP on PP. SP contributes to splanchnic vasodilatation in cirrhosis and this effect may be mediated by NO
机译:目的。 P(SP)物质是一种血管扩张剂,可能会导致肝硬化的全身和内脏血管扩张。这项研究的目的是确定肝硬化大鼠中SP(剂量-13 pg / kg)及其特异性抑制剂RP67580(剂量-300杯/ kg)对平均动脉压(MAP)和门静脉压(PP)的影响和控件。材料与方法。在施用SP和RP67580之前和之后测量MAP和PP。此外,在测量前,对一小群肝硬化大鼠进行L-NAME预处理,以阻断一氧化氮(NO)的作用。结果。 SP在两组中均产生短暂的系统性低血压。 SP导致肝硬化大鼠的PP明显增加,而对照组的PP减少。 RP67580降低了SP的降压作用,但没有完全降低。 RP67580降低肝硬化组的PP,但不降低对照组的PP。在用L-NAME预处理的肝硬化大鼠中,SP的给药导致MAP显着降低,而PP则无明显变化。结论外源性SP会增加肝硬化大鼠的PP并降低其MAP。 RP687580可以降低肝硬化大鼠的PP并降低SP引起的低血压。 NO封锁消除了SP对PP的影响。 SP有助于肝硬化内脏血管舒张,这种作用可能是由NO介导的

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