首页> 外文期刊>Japanese Journal of Pharmacology >BLOCKADE OF CARDIAC CALORIGENIC EFFECT OF EPINEPHRINE BY SOTALOL (MJ-1999)
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BLOCKADE OF CARDIAC CALORIGENIC EFFECT OF EPINEPHRINE BY SOTALOL (MJ-1999)

机译:Sotalol ePinephrine的心脏热量效应(MJ-1999)

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References(14) Cited-By(2) While the increase in cardiac work, force and rate are known to be a function of beta-adrenergic receptor stimulation, the mechanism of metabolic actions is uncertain. This study was undertaken to clarify the “calorigenic” action of epinephrine and its relation to hemodynamic changes. In a group of canine heart-lung preparations, the intra-atrial infusion of 0.01, 0.03 and 0.1 μg/kg of epinephrine did not change the cardiac work, force and rate, of the myocardial oxygen consumption, as compared to the control. However, intra-atrial infusion of 0.5 μg/kg of epinephrine caused an increase in cardiac work, cardiac isometric contraction, coronary flow and a marked elevation in the myocardial oxygen consumption above and beyond the rate of its effect on the cardiac hemodynamic parameters. Addition of 0.5 mg/kg of Sotalol did not cause depression of these parameters of left ventricular functions, including the coronary flow. However, 0.5 mg/kg of Sotalol effectively blocked the “calorigenic” action of 0.5 μg/kg of epinephrine. Apparently, more oxygen is being extracted by the myocardium after 0.5 μg/kg of epinephrine. Sotalol blocks this calorigenic action of epinephrine. Since the metabolic effects of epinephrine have not been shown to be beta-adrenergic receptor-mediated changes, it is concluded that Sotalol has the unique property of blocking the metabolic action of epinephrine.
机译:参考文献(14)引用(2),虽然已知心脏作品,力和速率的增加是β-肾上腺素能受体刺激的函数,但代谢行为的机制是不确定的。本研究阐明了肾上腺素的“热敏”作用及其与血流动力学变化的关系。在一组犬心脏肺准备中,与对照相比,心房内输注0.01,0.03和0.1μg/ kg肾上腺素没有改变心肌氧消耗的心脏作业,力和速率。然而,心房内输注0.5μg/ kg肾上腺素导致心脏作业,心脏等轴承收缩,冠状动脉血管率的增加,并且在心肌氧气消耗中的显着升高和超出其对心脏血流动力学参数的影响速率。添加0.5mg / kg的甲醇并未引起左心室功能的这些参数的抑郁,包括冠状动脉。然而,0.5mg / kg的sotalol有效地阻断了0.5μg/ kg肾上腺素的“热敏”作用。显然,在0.5μg/ kg肾上腺素后,心肌均提取更多的氧气。 Sotalol阻断了肾上腺素的这种热量作用。由于肾上腺素的代谢效应未被证明是β-肾上腺素能受体介导的变化,因此得出结论,Sotalol具有阻断肾上腺素代谢作用的独特性。

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