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吸入法舒地尔在血栓素诱导的新生羔羊急性肺动脉高压中缺乏肺选择性。

Inhaled Fasudil Lacks Pulmonary Selectivity in Thromboxane-Induced Acute Pulmonary Hypertension in Newborn Lambs.

作者信息

Hanson Shawn F L, Terry Michael H, Moretta Dafne T, Power Gordon G, Wilson Sean M, Alam Farzana, Ahsan Fakhrul, Blood Arlin B, Giri Paresh C

机构信息

1 Department of Pediatrics, Division of Neonatology, Loma Linda University School of Medicine, Loma Linda, CA, USA.

2 Department of Respiratory Care, Loma Linda University School of Medicine, Loma Linda, CA, USA.

出版信息

J Cardiovasc Pharmacol Ther. 2018 Sep;23(5):472-480. doi: 10.1177/1074248418772814. Epub 2018 May 13.

Abstract

INTRODUCTION

Pulmonary hypertension (PH) is a potentially deadly disease for infants and adults with few existing medical interventions and no cure. In PH, increased blood pressure in the pulmonary artery eventually leads to heart failure. Fasudil, an antagonist of Rho-kinase, causes vasodilation leading to decreased systemic artery pressure and pulmonary artery pressure (PAP). This study compared the effects of fasudil administered as either an intravenous infusion or inhaled aerosol in newborn lambs.

HYPOTHESIS

Inhaled aerosol delivery of fasudil will provide selective pulmonary vasodilation when compared with intravenous administration.

METHODS

Newborn lambs (∼11 days) were surgically instrumented and mechanically ventilated under anesthesia. A pulmonary artery catheter and ultrasonic flow probe were inserted to measure hemodynamics. Acute PH was pharmaceutically induced via continuous intravenous infusion of thromboxane. After achieving a 2- to 3-fold elevation of PAP, fasudil was administered either as intravenous infusion (2.5 mg/kg) or inhaled aerosol (100 mg of fasudil in 2 mL of saline). Changes in PAP, mean systemic arterial pressure (MABP), pulmonary vascular resistance (PVR), systemic vascular resistance (SVR), cardiac output, and heart rate were assessed. In addition, plasma concentrations of fasudil were measured.

RESULTS

Both routes of fasudil delivery produced significant decreases in PAP and PVR but also produced similar decreases in MABP and SVR. The C for intravenous fasudil was greater than that for inhaled fasudil.

CONCLUSIONS

These results suggest inhaled fasudil lacks pulmonary selectivity when compared with intravenous fasudil.

摘要

引言

肺动脉高压(PH)对于婴儿和成人来说是一种潜在的致命疾病,目前可用的医学干预措施很少,且无法治愈。在肺动脉高压中,肺动脉血压升高最终会导致心力衰竭。法舒地尔是一种Rho激酶拮抗剂,可引起血管舒张,导致体动脉血压和肺动脉压(PAP)降低。本研究比较了静脉输注或吸入气雾剂给药的法舒地尔对新生羔羊的影响。

假设

与静脉给药相比,吸入气雾剂形式的法舒地尔将提供选择性肺血管舒张作用。

方法

对新生羔羊(约11日龄)进行手术插管,并在麻醉下进行机械通气。插入肺动脉导管和超声流量探头以测量血流动力学。通过持续静脉输注血栓素药物诱导急性肺动脉高压。在肺动脉压升高2至3倍后,以静脉输注(2.5mg/kg)或吸入气雾剂(2mL生理盐水中含100mg法舒地尔)的方式给予法舒地尔。评估肺动脉压、平均体动脉压(MABP)、肺血管阻力(PVR)、体血管阻力(SVR)、心输出量和心率的变化。此外,还测量了法舒地尔的血浆浓度。

结果

两种法舒地尔给药途径均使肺动脉压和肺血管阻力显著降低,但也使平均体动脉压和体血管阻力出现类似程度的降低。静脉注射法舒地尔的曲线下面积大于吸入法舒地尔的曲线下面积。

结论

这些结果表明,与静脉注射法舒地尔相比,吸入法舒地尔缺乏肺选择性。

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