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环苯扎林毒性的五年多中心回顾性研究。

Five-year multicenter retrospective review of cyclobenzaprine toxicity.

作者信息

Spiller H A, Winter M L, Mann K V, Borys D J, Muir S, Krenzelok E P

机构信息

Kentucky Regional Poison Center, Kosair Children's Hospital, Louisville, KY 40232-5070, USA.

出版信息

J Emerg Med. 1995 Nov-Dec;13(6):781-5. doi: 10.1016/0736-4679(95)02019-5.

Abstract

Cyclobenzaprine (CBP) has a cyclic structure similar to amitriptyline. In overdose, CBP has been suggested to produce the cardiovascular and neurologic toxicity found with the cyclic antidepressants. To examine this possibility, a retrospective chart review of all cases of CBP exposure reported to five regional poison centers was performed for the years 1989-93. There were a total of 750 charts identified for CBP exposure, of which 523 had data sufficient for evaluation. There were 121 polydrug ingestions leaving 402 pure CBP ingestions. Ages ranged from 7 mo to 77 yrs, with a mean of 20 yrs; 26% were 6 yrs or less. Females comprised 63% of the patient group. No deaths occurred. Dysrhythmias beyond sinus tachycardia were infrequent, and none were life-threatening. No seizures occurred. Common effects were lethargy, sinus tachycardia, and agitation, and both hypertension and hypotension were seen. All symptomatic cases with a known time of ingestion were symptomatic within 4 h of ingestion. Doses ingested ranged from 5-1000 mg, with a mean of 133 mg. Asymptomatic and symptomatic patients had a mean dose ingested of 45 mg and 183 mg, respectively. Treatment was primarily gastrointestinal (GI) decontamination and supportive care. Other therapies required were mechanical ventilation, dopamine, fluid bolus, sedation, and foley catheter. Symptoms requiring treatment beyond GI decontamination did not occur with ingestions less than 100 mg. In conclusion, cyclobenzaprine does not appear to produce the life-threatening cardiovascular or neurologic effects of the cyclic antidepressants in doses less than 1 g. Lethargy and anticholinergic effects are prominent, though serious toxicity is infrequent.

摘要

环苯扎林(CBP)具有与阿米替林相似的环状结构。过量服用时,有人认为CBP会产生环状抗抑郁药所具有的心血管和神经毒性。为了探究这种可能性,对1989年至1993年期间向五个地区毒物中心报告的所有CBP暴露病例进行了回顾性图表审查。共识别出750例CBP暴露图表,其中523例有足够数据进行评估。有121例多药摄入,其余402例为单纯CBP摄入。年龄范围从7个月至77岁,平均年龄为20岁;26%为6岁及以下。女性占患者组的63%。无死亡病例。除窦性心动过速外的心律失常很少见,且无一例危及生命。无癫痫发作。常见症状为嗜睡、窦性心动过速和躁动,同时可见高血压和低血压。所有已知摄入时间的有症状病例在摄入后4小时内出现症状。摄入剂量范围为5 - 1000毫克,平均为133毫克。无症状和有症状患者的平均摄入剂量分别为45毫克和183毫克。治疗主要是胃肠道去污和支持性护理。所需的其他治疗包括机械通气、多巴胺、液体冲击、镇静和留置导尿管。摄入少于100毫克时,除胃肠道去污外无需其他治疗的症状未出现。总之,环苯扎林在剂量小于1克时似乎不会产生环状抗抑郁药那样危及生命的心血管或神经效应。嗜睡和抗胆碱能效应较为突出,不过严重毒性并不常见。

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