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清醒犬快速静脉注射罗哌卡因和布比卡因后急性全身毒性的治疗

Treatment of acute systemic toxicity after the rapid intravenous injection of ropivacaine and bupivacaine in the conscious dog.

作者信息

Feldman H S, Arthur G R, Pitkanen M, Hurley R, Doucette A M, Covino B G

机构信息

Department of Anesthesia Research Laboratories, Brigham and Women's Hospital, Harvard Medical School, Boston, Massachusetts.

出版信息

Anesth Analg. 1991 Oct;73(4):373-84.

PMID:1897763
Abstract

Two groups of six beagle dogs received rapid intravenous (IV) injections of ropivacaine or bupivacaine on two occasions in a blinded random fashion. Initially, a dose sufficient to cause convulsions (CD) was given followed by twice the CD (2 x CD), which was administered 48 h later. The CD of bupivacaine (4.3 mg/kg) and ropivacaine (4.9 mg/kg) caused significant (P less than 0.05) increases in heart rate and mean arterial blood pressure. There was no difference between drug groups. Seizures were abolished by 10 mg/kg of intravenous thiamylal. Endotracheal intubation and controlled respiration with O2-enriched air with no other treatment resulted in rapid and complete recovery in all dogs. All dogs receiving 2 x CD of bupivacaine (8.6 mg/kg) or ropivacaine (9.8 mg/kg) were initially treated with thiamylal and mechanical ventilation. Two dogs in the bupivacaine group developed hypotension, respiratory arrest, ventricular tachycardia, and ventricular fibrillation, which were resistant to closed chest cardiac massage, treatment with epinephrine, bretylium, and atropine, and direct current cardioversion. The four remaining dogs in the infusion group were successfully resuscitated. All of the animals in the ropivacaine-treated group survived the administration of the 2 x CD dose. Mild hypotension developed in one dog and was treated with intravenous epinephrine (0.75 mg). This resulted in nodal tachycardia, which was abolished after treatment with bretylium. Another dog had two 1-s bursts of premature ventricular contractions requiring no treatment. The rapid treatment of convulsions and cardiovascular toxicity resulted in a decreased number of deaths in both groups when compared with dogs from a previously published study in which no therapy was instituted. Thus, early aggressive treatment of central nervous system and cardiovascular system toxicity is capable of reducing the incidence of mortality associated with the rapid intravenous administration of excessive doses of local anesthetics.

摘要

两组各6只比格犬以双盲随机方式分两次接受了罗哌卡因或布比卡因的快速静脉注射。最初,给予足以引起惊厥的剂量(CD),然后在48小时后给予两倍的CD(2×CD)。布比卡因(4.3mg/kg)和罗哌卡因(4.9mg/kg)的CD剂量导致心率和平均动脉血压显著(P<0.05)升高。药物组之间无差异。10mg/kg静脉注射硫喷妥钠可消除惊厥。气管插管并用富氧空气进行控制呼吸,不进行其他治疗,所有犬均迅速完全恢复。所有接受2×CD剂量布比卡因(8.6mg/kg)或罗哌卡因(9.8mg/kg)的犬最初均接受硫喷妥钠和机械通气治疗。布比卡因组的两只犬出现低血压、呼吸骤停、室性心动过速和心室颤动,对胸外心脏按压、肾上腺素、溴苄铵和阿托品治疗以及直流电复律均无反应。输注组其余4只犬成功复苏。罗哌卡因治疗组的所有动物在给予2×CD剂量后均存活。一只犬出现轻度低血压,用静脉注射肾上腺素(0.75mg)治疗。这导致结性心动过速,用溴苄铵治疗后消失。另一只犬有两次1秒的室性早搏,无需治疗。与先前发表的未进行治疗的研究中的犬相比,惊厥和心血管毒性的快速治疗导致两组死亡数量减少。因此,对中枢神经系统和心血管系统毒性进行早期积极治疗能够降低与快速静脉注射过量局部麻醉药相关的死亡率。

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