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选择性多巴胺受体激动剂LY141865对全身血流动力学及局部血流的影响

Systemic hemodynamic and regional blood flow effects of LY141865, a selective dopamine receptor agonist.

作者信息

Hahn R A, MacDonald B R

出版信息

J Pharmacol Exp Ther. 1984 Sep;230(3):558-68.

PMID:6470973
Abstract

Intravenous infusion of LY141865 (20 micrograms/kg) lowered systemic vascular resistance in anesthetized dogs resulting in a fall in mean arterial blood pressure. These effects require an intact nervous system and involve dopamine receptors as they were abolished by hexamethonium or sulpiride pretreatment. LY141865 does not appear to interact with adrenergic receptors because it did not increase diastolic blood pressure or cardiac rate of normal or hexamethonium-treated dogs, and yohimbine pretreatment did not antagonize its systemic vasodilator and hypotensive actions. Hemodynamic analysis demonstrated that infusion of LY141865 (20 and 100 micrograms/kg i.v.) resulted in persistent arterial hypotension due solely to reduced systemic vascular resistance; aortic blood flow index was maintained. LY141865 produced slight bradycardia and sustained increments in stroke volume index at the highest tested dose. Left ventricular filling pressure was unchanged by LY141865. Regional blood flows to heart, stomach, colon, small intestine, kidneys and marrow-laden bone were not changed during hemodynamic alterations produced by LY141865, although evidence of arteriovenous shunting of blood was observed in skin and skeletal muscle. Comparable systemic vasodilation and arterial hypotension induced by infusion of nitroglycerin reduced gastric and colonic blood flows, but did not produce detectable shunting. The composite data are interpreted to be a reflection of the ability of LY141865 to interact with DA2 dopamine receptors and thereby inhibit neurogenic release of norepinephrine. The present results and known oral efficacy of LY141865 lend further support for the development and use of dopamine receptor agonists for the treatment of cardiovascular disease.

摘要

静脉注射LY141865(20微克/千克)可降低麻醉犬的全身血管阻力,导致平均动脉血压下降。这些作用需要完整的神经系统参与,且涉及多巴胺受体,因为六甲铵或舒必利预处理可消除这些作用。LY141865似乎不与肾上腺素能受体相互作用,因为它不会增加正常犬或六甲铵处理犬的舒张压或心率,且育亨宾预处理不会拮抗其全身血管舒张和降压作用。血流动力学分析表明,静脉注射LY141865(20和100微克/千克)仅因全身血管阻力降低而导致持续性动脉低血压;主动脉血流指数维持不变。在最高测试剂量下,LY141865产生轻微心动过缓并使每搏量指数持续增加。LY141865对左心室充盈压无影响。在LY141865引起的血流动力学改变过程中,心脏、胃、结肠、小肠、肾脏和富含骨髓的骨骼的局部血流量未发生变化,尽管在皮肤和骨骼肌中观察到血液动静脉分流的迹象。静脉注射硝酸甘油引起的类似全身血管舒张和动脉低血压可减少胃和结肠血流量,但未产生可检测到的分流。综合数据被解释为LY141865与DA2多巴胺受体相互作用并由此抑制去甲肾上腺素神经源性释放能力的反映。LY141865目前的结果和已知的口服疗效为多巴胺受体激动剂用于治疗心血管疾病的开发和使用提供了进一步支持。

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