Lalic Mladena, Cvejic Jelena, Popovic Jovan, Bozic Ksenija, Golocorbin-Kon Svetlana, Al-Salami Hani, Mikov Momir
Department of Pharmacy, Faculty of Medicine, Novi Sad, Republic of Serbia.
Eur J Drug Metab Pharmacokinet. 2009 Apr-Jun;34(2):93-9. doi: 10.1007/BF03191157.
Lamotrigine (LTG, 3,5-diamino-6- (2,3-dichlorphenyl)-,2,4-triazine) is an antiepileptic drug used mainly for partial and generalized seizures. The efficacy of LTG in treating resistant partial seizures was optimized when it was combined with valproate (VPA). The aim of this study was to investigate the influence of VPA on LTG pharmacokinetics in epileptic patients.
38 patients were randomly divided into two groups, one given LTG (n = 18) and the other given LTG + VPA(n = 20). The first group consisted of 10 females (32.50 +/- 12.46 years old, 67.80 +/- 15.18 kg) and 8 males (24.88 +/- 8.92 years old, 69.88 +/- 11.41 kg) and the second group consisted of 9 females (28.33 +/- 6.52 years old, 62.89 +/- 13.28 kg) and 11 males (37.64 +/- 10.43 years old, 85.64 +/- 15.4 kg). Patients were either administered an oral dose of LTG (157 +/- 74 mg/day) or LTG + VPA (150 +/- 83.11 mg/day & 774 +/- 330 mg/day respectively). LTG steady state serum concentrations were determined 1.5-8 h post dose. Analyses were performed by a validated HPLC method.
LTG serum concentrations were increased significantly from 4.67 +/- 3.66 and 9.56 +/- 5.27 microg/ml by concomitant administration of VPA.
The inhibition of LTG metabolism by VPA was shown to have a marked effect on LTG kinetics. This inhibitory effect was complicated further by inter-patients variation in body weight and gender. This emphasizes the importance of continuous monitoring of LTG serum concentrations on an individual basis. Accordingly, if the use of potentially interacting drugs cannot be avoided, adverse reactions can be minimized by dose adjustments guided by careful monitoring of clinical response and measurement of LTG serum concentrations.
拉莫三嗪(LTG,3,5 - 二氨基 - 6 - (2,3 - 二氯苯基) - 1,2,4 - 三嗪)是一种主要用于治疗部分性和全身性癫痫发作的抗癫痫药物。当拉莫三嗪与丙戊酸盐(VPA)联合使用时,其治疗耐药性部分性癫痫发作的疗效得到优化。本研究的目的是探讨丙戊酸盐对癫痫患者拉莫三嗪药代动力学的影响。
38例患者随机分为两组,一组给予拉莫三嗪(n = 18),另一组给予拉莫三嗪 + 丙戊酸盐(n = 20)。第一组包括10名女性(32.50±12.46岁,67.80±15.18 kg)和8名男性(24.88±8.92岁,69.88±11.41 kg),第二组包括9名女性(28.33±6.52岁,62.89±13.28 kg)和11名男性(37.64±10.43岁,85.64±15.4 kg)。患者分别口服拉莫三嗪(157±74 mg/天)或拉莫三嗪 + 丙戊酸盐(分别为150±83.11 mg/天和774±330 mg/天)。在给药后1.5 - 8小时测定拉莫三嗪稳态血清浓度。采用经过验证的高效液相色谱法进行分析。
联合使用丙戊酸盐后,拉莫三嗪血清浓度从4.67±3.66和9.56±5.27μg/ml显著升高。
丙戊酸盐对拉莫三嗪代谢的抑制作用对拉莫三嗪动力学有显著影响。这种抑制作用因患者体重和性别的个体差异而进一步复杂化。这强调了基于个体持续监测拉莫三嗪血清浓度的重要性。因此,如果无法避免使用可能相互作用的药物,通过仔细监测临床反应和测定拉莫三嗪血清浓度来指导剂量调整,可以将不良反应降至最低。
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