Mathier Michael A, Shen You-Tang, Shannon Richard P
Cardiovascular Institute of the University of Pittsburgh Health System, University of Pittsburgh School of Medicine, Pittsburgh, Pennsylvania 15213, USA.
J Card Fail. 2002 Dec;8(6):407-15. doi: 10.1054/jcaf.2002.129233.
The aim of this study was to explore the characteristics and mechanisms of the cardiovascular effects of cocaine in dilated cardiomyopathy.
We studied the cardiovascular responses to acute intravenous cocaine (1 mg/kg) in 8 conscious, chronically instrumented dogs before and after the development of dilated cardiomyopathy induced by rapid ventricular pacing. To help elucidate the role of altered baroreflex function in mediating the cardiovascular effects of cocaine, we also studied responses in 3 conscious, chronically instrumented dogs that had undergone surgical sinoaortic baroreceptor denervation. Cocaine produced greater increases in heart rate (+57 +/- 8% from 112 +/- 5 beats/min versus +28 +/- 3% from 100 +/- 4 beats/min; P <.01), first derivative of left ventricular pressure (+30 +/- 5% from 1,714 +/- 147 mm Hg/sec versus +15 +/- 3% from 3,032 +/- 199 mm Hg/sec; P <.01), coronary vascular resistance (+28 +/- 5% from 2.3 +/- 0.3 mm Hg/mL/min versus +11 +/- 5% from 2.2 +/- 0.3 mm Hg/mL/min; P <.05) and plasma norepinephrine concentration (+130 +/- 31% from 462 +/- 102 pg/mL versus +86 +/- 32% from 286 +/- 77 pg/mL; P <.05) in dogs with dilated cardiomyopathy as compared to controls. In addition, responses were much more rapid in onset following the development of dilated cardiomyopathy. Chronotropic and inotropic responses to cocaine were similarly rapid and exaggerated in dogs after baroreceptor denervation.
Cocaine produces rapid and exaggerated chronotropic, inotropic, and coronary vasoconstrictor responses in conscious dogs with pacing-induced dilated cardiomyopathy. Alterations in arterial baroreflex function may play a role in these observations, which in turn may underlie the clinically observed association between cocaine and heart failure.
本研究旨在探讨可卡因对扩张型心肌病心血管影响的特征及机制。
我们研究了8只清醒的、长期植入仪器的犬在快速心室起搏诱导扩张型心肌病前后,静脉注射急性可卡因(1毫克/千克)后的心血管反应。为了阐明压力感受性反射功能改变在介导可卡因心血管效应中的作用,我们还研究了3只清醒的、长期植入仪器且已接受手术去主动脉弓压力感受器神经支配的犬的反应。与对照组相比,扩张型心肌病犬注射可卡因后心率升高幅度更大(从112±5次/分钟升高57±8%,而对照组从100±4次/分钟升高28±3%;P<.01),左心室压力一阶导数升高幅度更大(从1714±147毫米汞柱/秒升高30±5%,而对照组从3032±199毫米汞柱/秒升高15±3%;P<.01),冠状血管阻力升高幅度更大(从2.3±0.3毫米汞柱/毫升/分钟升高28±5%,而对照组从2.2±0.3毫米汞柱/毫升/分钟升高11±5%;P<.05),血浆去甲肾上腺素浓度升高幅度更大(从462±102皮克/毫升升高130±3l%,而对照组从286±77皮克/毫升升高86±32%;P<.05)。此外,扩张型心肌病发生后,反应起效更快。压力感受器去神经支配的犬对可卡因的变时性和变力性反应同样迅速且增强。
可卡因在起搏诱导的扩张型心肌病清醒犬中产生迅速且增强的变时性、变力性和冠状血管收缩反应。动脉压力感受性反射功能改变可能在这些观察结果中起作用,这反过来可能是临床上观察到的可卡因与心力衰竭之间关联的基础。
Zotero 插件