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抗惊厥药对人类受试者和实验动物中氟烷诱导的肝损伤的影响。

Effects of anticonvulsant agents on halothane-induced liver injury in human subjects and experimental animals.

作者信息

Nomura F, Hatano H, Ohnishi K, Akikusa B, Okuda K

出版信息

Hepatology. 1986 Sep-Oct;6(5):952-6. doi: 10.1002/hep.1840060523.

Abstract

In order to evaluate the clinical implication of experimental studies on halothane-induced liver damage in phenobarbital-treated rats, we studied the clinical records of 315 consecutive patients who underwent brain surgery with halothane anesthesia. After exclusion of subjects with a history of alcoholism or antecedent chronic liver disease, clinical data of 279 patients with normal preoperative transaminase activities were analyzed. The incidence of halothane-induced liver injury was significantly higher in the subjects given phenobarbital than in those with no phenobarbital medication (7/100 vs. 1/179, p less than 0.01). To determine if other anticonvulsant compounds can influence halothane-induced liver injury, rats were pretreated with diphenylhydantoin or valproic acid prior to exposure to halothane under hypoxic conditions for comparison with phenobarbital. The degree of halothane hepatotoxicity assessed from ALT activities and morphological alterations was of the decreasing order of phenobarbital greater than controls = diphenylhydantoin greater than valproic acid, and a similar order was observed in the extent of reductive metabolism of halothane. These results indicate that patients pretreated with phenobarbital may be at a greater risk of halothane-induced liver damage, and that treatment with valproic acid and diphenylhydantoin lead to the production of toxic intermediates of halothane to a lesser extent than treatment with phenobarbital does.

摘要

为了评估在苯巴比妥处理的大鼠中关于氟烷诱导肝损伤的实验研究的临床意义,我们研究了315例连续接受氟烷麻醉下脑手术患者的临床记录。在排除有酗酒史或先前慢性肝病病史的受试者后,分析了279例术前转氨酶活性正常患者的临床资料。接受苯巴比妥治疗的受试者中氟烷诱导肝损伤的发生率显著高于未服用苯巴比妥的受试者(7/100对1/179,p<0.01)。为了确定其他抗惊厥化合物是否会影响氟烷诱导的肝损伤,在缺氧条件下,大鼠在接触氟烷之前先用苯妥英或丙戊酸预处理,以便与苯巴比妥进行比较。从ALT活性和形态学改变评估的氟烷肝毒性程度顺序为苯巴比妥>对照组=苯妥英>丙戊酸,并且在氟烷的还原代谢程度方面也观察到类似顺序。这些结果表明,接受苯巴比妥预处理的患者可能有更高的氟烷诱导肝损伤风险,并且与苯巴比妥治疗相比,丙戊酸和苯妥英治疗导致氟烷毒性中间体产生的程度较小。

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