Kramer Anders, Mortensen Christian Schmidt, Schultz Jacob Gammelgaard, Lyhne Mads Dam, Andersen Asger, Nielsen-Kudsk Jens Erik
Department of Cardiology, Aarhus University Hospital, Aarhus, Denmark.
Department of Clinical Medicine, Faculty of Health, Aarhus University, Aarhus, Denmark.
Eur Heart J Acute Cardiovasc Care. 2021 May 11;10(3):265–272. doi: 10.1177/2048872620918713. Epub 2020 Jul 14.
Inhaled nitric oxide (iNO) effectively reduces right ventricular afterload when administered in the immediate phase of acute pulmonary embolism (PE) in preclinical animal models. In a porcine model of intermediate-risk PE, we aimed to investigate whether iNO has pulmonary vasodilator efficacy both in the immediate and prolonged phase of acute PE.
Anesthetized pigs ( = 18) were randomized into three subgroups. An acute PE iNO-group ( = 6) received iNO at 40 ppm at one, three, six, nine and 12 hours after onset of PE. Vehicle animals ( = 6) received PE, but no active treatment. A third group of sham animals ( = 6) received neither PE nor treatment. Animals were evaluated using intravascular pressures, respiratory parameters, biochemistry and intracardiac pressure-volume measurements.
The administration of PE increased mean pulmonary artery pressure (mPAP) (vehicle vs sham; 33.3 vs 17.7 mmHg, < 0.0001), pulmonary vascular resistance (vehicle vs sham; 847.5 vs 82.0 dynes, < 0.0001) and right ventricular arterial elastance (vehicle vs sham; 1.2 vs 0.2 mmHg/ml, < 0.0001). Significant mPAP reduction by iNO was preserved at 12 hours after the onset of acute PE (vehicle vs iNO; 0.5 vs -3.5 mmHg, < 0.0001). However, this response was attenuated over time ( = 0.0313). iNO did not affect the systemic circulation.
iNO is a safe and effective pulmonary vasodilator both in the immediate and prolonged phase of acute PE in an in-vivo porcine model of intermediate-risk PE.
在临床前动物模型中,吸入一氧化氮(iNO)在急性肺栓塞(PE)的即刻阶段给药时可有效降低右心室后负荷。在中度风险PE的猪模型中,我们旨在研究iNO在急性PE的即刻和延长阶段是否具有肺血管舒张功效。
将18只麻醉猪随机分为三个亚组。急性PE iNO组(n = 6)在PE发作后1、3、6、9和12小时接受40 ppm的iNO。载体动物组(n = 6)接受PE,但未进行积极治疗。第三组假手术动物组(n = 6)既未接受PE也未接受治疗。使用血管内压力、呼吸参数、生物化学和心内压力-容积测量对动物进行评估。
PE给药增加了平均肺动脉压(mPAP)(载体组与假手术组;33.3 vs 17.7 mmHg,P < 0.0001)、肺血管阻力(载体组与假手术组;847.5 vs 82.0达因,P < 0.0001)和右心室动脉弹性(载体组与假手术组;1.2 vs 0.2 mmHg/ml,P < 0.0001)。急性PE发作后12小时,iNO对mPAP的显著降低作用得以维持(载体组与iNO组;0.5 vs -3.5 mmHg,P < 0.0001)。然而,这种反应随时间减弱(P = 0.0313)。iNO不影响体循环。
在中度风险PE的体内猪模型中,iNO在急性PE的即刻和延长阶段均是一种安全有效的肺血管舒张剂。
