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Vasopressin intravenous infusion causes dose dependent adverse cardiovascular effects in anesthetized dogs

机译:加压素静脉输注可引起麻醉犬剂量依赖性心血管不良反应

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摘要

BACKGROUND: Arginine vasopressin (AVP) has been broadly used in the management of vasodilatory shock. However, there are many concerns regarding its clinical use, especially in high doses, as it can be associated with adverse cardiovascular events. OBJECTIVE: To investigate the cardiovascular effects of AVP in continuous IV infusion on hemodynamic parameters in dogs. METHODS: Sixteen healthy mongrel dogs, anesthetized with pentobarbital were intravascularly catheterized, and randomly assigned to: control (saline-placebo; n=8) and AVP (n=8) groups. The study group was infused with AVP for three consecutive 10-minute periods at logarithmically increasing doses (0.01; 0.1 and 1.0U/kg/min), at them 20-min intervals. Heart rate (HR) and intravascular pressures were continuously recorded. Cardiac output was measured by the thermodilution method. RESULTS: No significant hemodynamic effects were observed during 0.01U/kg/min of AVP infusion, but at higher doses (0.1 and 1.0U/kg/min) a progressive increase in mean arterial pressure (MAP) and systemic vascular resistance index (SVRI) were observed, with a significant decrease in HR and the cardiac index (CI). A significant increase in the pulmonary vascular resistance index (PVRI) was also observed with the 1.0U/kg/min dose, mainly due to the decrease in the CI. CONCLUSION: AVP, when administered at doses between 0.1 and 1.0U/kg/min, induced significant increases in MAP and SVRI, with negative inotropic and chronotropic effects in healthy animals. Although these doses are ten to thousand times greater than those routinely used for the management of vasodilatory shock, our data confirm that AVP might be used carefully and under strict hemodynamic monitoring in clinical practice, especially if doses higher than 0.01 U/kg/min are needed.
机译:背景:精氨酸加压素(AVP)已被广泛用于血管舒张性休克的治疗。但是,由于其可能与不良的心血管事件有关,因此其临床用途存在很多担忧,尤其是在大剂量情况下。目的:探讨连续静脉输注AVP对犬血液动力学参数的心血管影响。方法:将十六只健康的杂种狗用戊巴比妥麻醉,并在血管内导管插入,随机分为对照组(盐水安慰剂; n = 8)和AVP(n = 8)组。对研究组连续三个10分钟以对数增加的剂量(0.01; 0.1和1.0U / kg / min)输注AVP,间隔为20分钟。连续记录心率(HR)和血管内压力。通过热稀释法测量心输出量。结果:在0.01U / kg / min的AVP输注过程中未观察到明显的血液动力学影响,但在更高剂量(0.1和1.0U / kg / min)下,平均动脉压(MAP)和全身血管阻力指数(SVRI)逐渐升高),HR和心脏指数(CI)明显下降。剂量为1.0U / kg / min时,肺血管阻力指数(PVRI)也显着增加,这主要是由于CI降低所致。结论:AVP以0.1至1.0U / kg / min的剂量给药时,可导致MAP和SVRI显着增加,对健康动物的正性和变时性都有负面影响。尽管这些剂量比处理血管扩张性休克的常规剂量大十至千倍,但我们的数据证实,在临床实践中,AVP可能会谨慎使用并在严格的血液动力学监测下使用,尤其是当剂量大于0.01 U / kg / min时。需要。

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