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丙戊酸盐与卡马西平联合用药会改变癫痫儿童血清中的肝酶活性。

Valproate and carbamazepine comedication changes hepatic enzyme activities in sera of epileptic children.

作者信息

Cepelak I, Zanić Grubisić T, Mandusić A, Rekić B, Lenicek J

机构信息

Department of Medical Biochemistry and Haematology, Faculty of Pharmacy and Biochemistry, University of Zagreb, Croatia.

出版信息

Clin Chim Acta. 1998 Aug 28;276(2):121-7. doi: 10.1016/s0009-8981(98)00094-1.

Abstract

Previous observation that valproic acid (VPA) and carbamazepine (CBZ) caused hepatic damage prompted us to investigate the effects of VPA or CBZ monotherapy and VPA + CBZ comedication on the number of hepatic enzyme activities in sera of epileptic children. This study compares alanine aminotransferase (ALT), aspartate aminotransferase (AST) and gamma-glutamyltransferase (GGT) activities in sera of children treated with VPA (n=42), or CBZ (n=36) taken as a monotherapy, with VPA + CBZ combined therapy (n=36). The effect of VPA alone is greater on the activity of AST than on other enzymes, while CBZ therapy changes primarily the activities of GGT. The mean catalytic activity of AST was significantly elevated in groups on VPA, CBZ and VPA + CBZ treatment (2.02-, 1.49- and 1.45-fold increase, respectively) as compared to the control values. Changes in the ALT activity followed different patterns. The maximal increase was observed in the CBZ group with a smaller increase in the group on VPA + CBZ polytherapy, whereas only 15% of patients receiving VPA showed an average 1.38-fold increase of the mean enzyme activity. Increase in the catalytic activity of GGT probably reflects the induction produced by the CBZ treatment, either alone or in combination. Children on CBZ monotherapy showed an increase of mean catalytic activity of about twofold in 56% of patients. Children on VPA + CBZ comedication showed a similar behaviour, while VPA alone produced a moderate (1.44-fold) increase in 23% of children. However, concentrations of VPA and CBZ in sera of patients receiving monotherapy were within the expected therapeutic limits, whereas subtherapeutic levels of VPA were found in 30% of children on VPA + CBZ comedication. We propose that individual dosage adjustment in VPA + CBZ polytherapy should be combined with monitoring of relevant enzyme activities in serum.

摘要

先前观察到丙戊酸(VPA)和卡马西平(CBZ)会导致肝损伤,这促使我们研究VPA或CBZ单药治疗以及VPA + CBZ联合用药对癫痫儿童血清中肝酶活性数量的影响。本研究比较了接受VPA单药治疗(n = 42)、CBZ单药治疗(n = 36)以及VPA + CBZ联合治疗(n = 36)的儿童血清中的丙氨酸氨基转移酶(ALT)、天冬氨酸氨基转移酶(AST)和γ-谷氨酰转移酶(GGT)活性。单独使用VPA对AST活性的影响大于对其他酶的影响,而CBZ治疗主要改变GGT的活性。与对照值相比,接受VPA、CBZ和VPA + CBZ治疗的组中AST的平均催化活性显著升高(分别增加2.02倍、1.49倍和1.45倍)。ALT活性的变化遵循不同模式。CBZ组观察到最大增幅,VPA + CBZ联合治疗组增幅较小,而仅15%接受VPA治疗的患者平均酶活性增加了1.38倍。GGT催化活性的增加可能反映了CBZ单独或联合治疗产生的诱导作用。接受CBZ单药治疗的儿童中,56%的患者平均催化活性增加了约两倍。接受VPA + CBZ联合治疗的儿童表现出类似情况,而单独使用VPA时,23%的儿童有中度增加(1.44倍)。然而,接受单药治疗的患者血清中VPA和CBZ的浓度在预期治疗范围内,而在接受VPA + CBZ联合治疗的儿童中,30%的儿童VPA水平低于治疗水平。我们建议,VPA + CBZ联合治疗中的个体剂量调整应结合监测血清中相关酶的活性。

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