Interactions between antiepileptic drugs, and between antiepileptic drugs and other drugs

被引:227
|
作者
Zaccara, Gaetano [1 ]
Perucca, Emilio [2 ,3 ]
机构
[1] Florence Hlth Author, Dept Med, Neurol Unit, Florence, Italy
[2] Univ Pavia, Dept Internal Med & Therapeut, I-27100 Pavia, Italy
[3] C Mondino Natl Neurol Inst, Pavia, Italy
关键词
antiepileptic drugs; epilepsy; drug interactions; pharmacokinetics; pharmacodynamics; humans; STEADY-STATE PHARMACOKINETICS; PLASMA CLOZAPINE CONCENTRATIONS; ENZYME-INDUCING ANTIEPILEPTICS; ACID SERUM CONCENTRATIONS; HEALTHY MALE-SUBJECTS; VALPROIC ACID; MONITORING SERVICE; CLINICAL PHARMACOKINETICS; BIPOLAR DISORDER; OPEN-LABEL;
D O I
10.1684/epd.2014.0714
中图分类号
R74 [神经病学与精神病学];
学科分类号
摘要
Interactions between antiepileptic drugs, or between antiepileptic drugs and other drugs, can be pharmacokinetic or pharmacodynamic in nature. Pharmacokinetic interactions involve changes in absorption, distribution or elimination, whereas pharmacodynamic interactions involve synergism and antagonism at the site of action. Most clinically important interactions of antiepileptic drugs result from induction or inhibition of drug metabolism. Carbamazepine, phenytoin, phenobarbital and primidone are strong inducers of cytochrome P450 and glucuronizing enzymes (as well as P-glycoprotein) and can reduce the efficacy of co-administered medications such as oral anticoagulants, calcium antagonists, steroids, antimicrobial and antineoplastic drugs through this mechanism. Oxcarbazepine, eslicarbazepine acetate, felbamate, rufinamide, topiramate (at doses 200 mg/day) and perampanel (at doses 8 mg/day) have weaker inducing properties, and a lower propensity to cause interactions mediated by enzyme induction. Unlike enzyme induction, enzyme inhibition results in decreased metabolic clearance of the affected drug, the serum concentration of which may increase leading to toxic effects. Examples of important interactions mediated by enzyme inhibition include the increase in the serum concentration of phenobarbital and lamotrigine caused by valproic acid. There are also interactions whereby other drugs induce or inhibit the metabolism of antiepileptic drugs, examples being the increase in serum carbamazepine concentration by erythromycin, and the decrease in serum lamotrigine concentration by oestrogen-containing contraceptives. Pharmacodynamic interactions between antiepileptic drugs may also be clinically important. These interactions can have potentially beneficial effects, such as the therapeutic synergism of valproic acid combined with lamotrigine, or adverse effects, such as the reciprocal potentiation of neurotoxicity observed in patients treated with a combination of sodium channel blocking antiepileptic drugs.
引用
收藏
页码:409 / 431
页数:23
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