Ayoub Iyad M, Kolarova Julieta, Kantola Ronald L, Sanders Robert, Gazmuri Raúl J
Department of Medicine, Rosalind Franklin University of Medicine and Science, USA.
Crit Care Med. 2005 Nov;33(11):2599-605. doi: 10.1097/01.ccm.0000186773.88576.83.
Epinephrine given during closed-chest resuscitation increases blood flow across the coronary and cerebral circuits. However, epinephrine worsens reperfusion arrhythmias and intensifies postresuscitation myocardial dysfunction. We investigated whether cariporide-a selective sodium-hydrogen exchanger isoform-1 inhibitor-could ameliorate such adverse effects without diminishing its vasopressor actions.
Randomized animal study.
University-based animal laboratory.
Twenty-four anesthetized male domestic pigs (29-43 kg).
Ventricular fibrillation was electrically induced and left untreated for 8 mins. Pigs were randomized to receive after 2 mins of chest compression a 3 mg/kg bolus of cariporide (n = 8), a 0.02 mg/kg bolus of epinephrine (n = 8), or a combination of cariporide and epinephrine (n = 8). Additional doses of epinephrine were given if the coronary perfusion pressure decreased below 15 mm Hg. Successfully resuscitated pigs were observed for 72 hrs.
The averaged coronary perfusion pressure was higher in the epinephrine (34 +/- 11 mm Hg, p = .001) and cariporide/epinephrine (35 +/- 10 mm Hg, p < .001) groups compared with the cariporide group (15 +/- 6 mm Hg). All pigs in the epinephrine and cariporide/epinephrine groups but only six in the cariporide group were successfully resuscitated and survived 72 hrs. During the immediate postresuscitation period, four of eight pigs in the epinephrine group had episodes of recurrent ventricular fibrillation or pulseless ventricular tachycardia requiring additional electrical shocks (7.0 +/- 6.4) but none in the cariporide and cariporide/epinephrine groups (chi-square, p = .008). Myocardial dysfunction occurred early after return of spontaneous circulation but only in the epinephrine group.
The combined administration of cariporide and epinephrine prompted adequate pressor effects during chest compression and facilitated reestablishment of cardiac activity without episodes of recurrent ventricular fibrillation or transient myocardial dysfunction as with epinephrine alone.
在闭胸复苏期间给予肾上腺素可增加冠状动脉和脑循环的血流量。然而,肾上腺素会加重再灌注心律失常并加剧复苏后心肌功能障碍。我们研究了卡里波罗德(一种选择性钠氢交换体同工型1抑制剂)是否能在不减弱其升压作用的情况下改善这些不良反应。
随机动物研究。
大学动物实验室。
24只麻醉的雄性家猪(体重29 - 43千克)。
电诱导室颤并持续8分钟不予处理。在进行2分钟胸外按压后,猪被随机分为三组,分别接受3毫克/千克的卡里波罗德静脉推注(n = 8)、0.02毫克/千克的肾上腺素静脉推注(n = 8)或卡里波罗德与肾上腺素联合使用(n = 8)。如果冠状动脉灌注压降至15毫米汞柱以下,则给予额外剂量的肾上腺素。成功复苏的猪观察72小时。
与卡里波罗德组(15 ± 6毫米汞柱)相比,肾上腺素组(34 ± 11毫米汞柱,p = 0.001)和卡里波罗德/肾上腺素组(35 ± 10毫米汞柱,p < 0.001)的平均冠状动脉灌注压更高。肾上腺素组和卡里波罗德/肾上腺素组的所有猪均成功复苏并存活72小时,而卡里波罗德组只有6只成功复苏。在复苏后的即刻阶段,肾上腺素组8只猪中有4只出现反复室颤或无脉性室性心动过速发作,需要额外电击(7.0 ± 6.4次),而卡里波罗德组和卡里波罗德/肾上腺素组均无此情况(卡方检验,p = 0.008)。自主循环恢复后早期出现心肌功能障碍,但仅在肾上腺素组出现。
卡里波罗德与肾上腺素联合使用在胸外按压期间产生了足够
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