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在麦角腈心血管作用中突触前多巴胺受体的刺激作用

Presynaptic dopamine receptor stimulation in the cardiovascular actions of lergotrile.

作者信息

Barrett R J, Lokhandwala M F

出版信息

J Pharmacol Exp Ther. 1981 Jun;217(3):660-5.

PMID:6112262
Abstract

The involvement of dopamine receptors present at different sites in the hypotensive and bradycardic actions of lergotrile was investigated. Intravenous administration of lergotrile to pentobarbital-anesthetized dogs decreased blood pressure, heart rate and renal vascular resistance and increased renal blood flow. These effects were prevented by prior treatment with sulpiride or with hexamethonium plus atropine. When administered to phentolamine-treated animals, lergotrile failed to alter either blood pressure or renal blood flow, but exerted and an enhanced bradycardic effect. Lergotrile significantly inhibited the positive chronotropic and renal vasoconstrictor effects elicited by cardiac and renal sympathetic nerve stimulation, which could be prevented by prior treatment with sulpiride, suggesting that stimulation of presynaptic dopamine receptors was responsible for the inhibition of sympathetic nerve function caused by lergotrile. Administration of lergotrile into the vertebral artery did not produce any cardiovascular changes, whereas i.c.v. lergotrile caused a transient tachycardia followed by a bradycardia of greater magnitude and duration than that seen after i.v. administration. These studies suggest that lergotrile exerts its hypotensive and bradycardiac effects via stimulation of presynaptic dopamine receptors resulting in subsequent inhibition of sympathetic nerve function. Dopamine receptors present in the brain may contribute to the bradycardia, but vascular dopamine receptors do not appear to be involved in the cardiovascular actions of lergotrile.

摘要

研究了不同部位的多巴胺受体在麦角腈降压和减慢心率作用中的参与情况。对戊巴比妥麻醉的犬静脉注射麦角腈可降低血压、心率和肾血管阻力,并增加肾血流量。这些作用可被事先用舒必利或六甲铵加阿托品处理所阻断。当给酚妥拉明处理的动物注射麦角腈时,它未能改变血压或肾血流量,但产生了增强的减慢心率作用。麦角腈显著抑制心脏和肾交感神经刺激所引起的正性变时作用和肾血管收缩作用,事先用舒必利处理可阻断这种作用,这表明突触前多巴胺受体的刺激是麦角腈引起交感神经功能抑制的原因。将麦角腈注入椎动脉未产生任何心血管变化,而脑室内注射麦角腈则引起短暂的心动过速,随后出现的心动过缓比静脉注射后更明显且持续时间更长。这些研究表明,麦角腈通过刺激突触前多巴胺受体发挥其降压和减慢心率作用,从而导致随后交感神经功能的抑制。脑内存在的多巴胺受体可能与心动过缓有关,但血管多巴胺受体似乎不参与麦角腈的心血管作用。

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