Mink S N, Simons F E R, Simons K J, Becker A B, Duke K
Department of Medicine and Pharmacology and Therapeutics, University of Manitoba, Winnipeg, MB, Canada.
Clin Exp Allergy. 2004 Nov;34(11):1776-83. doi: 10.1111/j.1365-2222.2004.02106.x.
Epinephrine (Epi) is the treatment of choice for reversing cardiovascular collapse in anaphylactic shock (AS). In this condition, most treatment guidelines have been anecdotally derived and no randomized clinical trials have been conducted. In the present study, we examined the time course of haemodynamic recovery in a canine model of AS when Epi was administered at the initiation of allergen challenge before fully developed shock had occurred.
Randomized, controlled, crossover studies were performed approximately 3-5 weeks apart in ragweed-sensitized dogs while the animals were ventilated and anaesthetized. Epi was administered by bolus intravenous (i.v.), subcutaneous (s.c.), intramuscular (i.m.) routes and by continuous i.v. infusion (CI). The findings obtained in the Epi treatment (T) studies were compared with those found in a no treatment (NT) study. In the bolus studies, Epi was administered at 0.01 mg/kg, while in the CI study, the dose of Epi was titrated to maintain mean arterial pressure (MAP) at 70% of preshock levels. MAP, cardiac output (CO), stroke volume (SV), and pulmonary wedge pressure (Pwp) were determined over a 3 h period.
In the CI study, haemodynamics (CO, MAP, and SV) were significantly higher than those measured in the NT study and the bolus studies over approximately the first hour of the study. In the CI study, the amount of Epi infused was significantly less than in the bolus studies.
When administered at the initiation of allergen challenge, bolus treatment of Epi by i.m., i.v., or s.c. routes caused limited haemodynamic improvement in AS. In contrast, constant infusion of Epi at a lower total dose produced significant haemodynamic improvement. Within the limits of this anaesthetized canine model, the results suggest that CI should be the preferred route in the treatment of AS when this treatment option is available.
肾上腺素(Epi)是过敏性休克(AS)中逆转心血管衰竭的首选治疗药物。在这种情况下,大多数治疗指南都是基于轶事得出的,尚未进行随机临床试验。在本研究中,我们研究了在变应原激发开始时、休克完全发展之前给予Epi的犬AS模型中血流动力学恢复的时间过程。
在豚草致敏犬中,每隔约3 - 5周进行一次随机、对照、交叉研究,同时对动物进行通气和麻醉。Epi通过静脉推注(i.v.)、皮下(s.c.)、肌肉注射(i.m.)途径以及静脉持续输注(CI)给药。将Epi治疗(T)研究中获得的结果与未治疗(NT)研究中发现的结果进行比较。在推注研究中,Epi以0.01 mg/kg给药,而在CI研究中,Epi的剂量进行滴定以将平均动脉压(MAP)维持在休克前水平的70%。在3小时内测定MAP、心输出量(CO)、每搏输出量(SV)和肺楔压(Pwp)。
在CI研究中,在研究的大约第一个小时内,血流动力学指标(CO、MAP和SV)显著高于NT研究和推注研究中测得的指标。在CI研究中,输注的Epi量显著少于推注研究。
在变应原激发开始时给药,通过i.m.、i.v.或s.c.途径推注治疗Epi在AS中引起的血流动力学改善有限。相比之下,以较低的总剂量持续输注Epi可产生显著的血流动力学改善。在这个麻醉犬模型的限制范围内,结果表明当有这种治疗选择时,CI应该是AS治疗的首选途径。
