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Carbamazepine-10,11-epoxide in therapeutic drug monitoring.

机译:卡马西平-10,11-环氧化物在治疗药物监测中。

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Carbamazepine (CBZ) is widely used in the treatment of epilepsy, frequently in combination with other anticonvulsants. Its metabolite, carbamazepine-10,11-epoxide, is pharmacologically active and is increased with concurrent use of valproate and other anticonvulsants. This pharmacokinetic interaction may be particularly important because CBZ, its epoxide, phenytoin, and lamotrigine all act on fast voltage-dependent sodium channels. Over a 2-month period, routine serum requests for CBZ (n=47) (excluding known cases of overdose) were also analyzed for CBZ epoxide, phenytoin, and lamotrigine using a simultaneous high performance liquid chromatographic (HPLC) method. Valproate was measured using fluorescence polarization immunoassay (FPIA). With concurrent phenytoin and lamotrigine administration, there was a relative increase in CBZ epoxide and a significant decrease in the ratio of CBZ to epoxide (from more than 5 to 3). If valproate was also present, the concentration of parent and metabolite increased significantly, causing potential toxicity. Two patients in this latter group had significant clinical toxicity, with parent CBZ concentrations in the reference range; a third patient suffered from poor control of seizures. This study illustrates the importance of awareness of the contribution of active metabolites in therapeutic drug monitoring and raises questions about the role of the routine monitoring of such metabolites.
机译:卡马西平(CBZ)通常与其他抗惊厥药联合用于癫痫的治疗。它的代谢物卡马西平-10,11-环氧化物具有药理活性,并同时使用丙戊酸盐和其他抗惊厥药时会增加。这种药代动力学的相互作用可能尤其重要,因为CBZ,其环氧化合物,苯妥英钠和拉莫三嗪均作用于快速的电压依赖性钠通道。在两个月的时间内,还使用同时高效液相色谱(HPLC)方法分析了常规CBZ血清要求(n = 47)(不包括已知的过量药物),以分析CBZ环氧化物,苯妥英钠和拉莫三嗪。使用荧光偏振免疫测定法(FPIA)测定丙戊酸盐。苯妥英钠和拉莫三嗪同时给药时,CBZ环氧化物相对增加,CBZ与环氧化物之比显着降低(从5降至3)。如果还存在丙戊酸酯,则母体和代谢产物的浓度会显着增加,从而引起潜在的毒性。后一组中有两名患者具有明显的临床毒性,其母体CBZ浓度在参考范围内。第三名患者癫痫发作控制不佳。这项研究说明了认识活性代谢物在治疗药物监测中的重要性,并提出了有关此类代谢物常规监测作用的疑问。

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