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Clinical effects of topiramate against secondarily generalized tonic-clonic seizures.

机译:托吡酯对抗继发性强直阵挛性癫痫发作的临床效果。

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OBJECTIVE: Intensive and quantitative evaluation of the duration, intensity and frequency of tonic and clonic signs of secondarily generalized tonic-clonic seizures (GTCS) in patients with pharmacoresistant partial seizures during topiramate (TPM) treatment. METHODS: Thirty patients suffering from refractory partial seizures with secondarily GTCS undergoing presurgical evaluation were randomized into a low dosage (100 mg daily) and a parallel medium dosage (200 mg daily) group of TPM add-on medication (15 patients for each group). Study phases included a 3 days baseline video-EEG phase, a 10 days TPM titration phase without video-EEG and a 3 days TPM dose maintenance phase with video-EEG. During the baseline and the dose maintenance phase seizures were recorded using video-EEG monitoring and the following parameters were measured for each recorded secondarily generalized tonic and clonic signs: duration (lasting seconds), intensity (on a 0-3 scale), frequency (numbers per 24 h). RESULTS: A total of 46 complex partial seizures with secondarily generalized tonic-clonic signs during the baseline phase and 20 during the dose maintenance phase were intensively analyzed. More patients in the medium dosage group than in the low dosage groups were free from secondarily GTCS during the dose maintenance phase (nine vs. two, P<0.05). Intergroup comparison suggested that the duration of all tonic signs decreased more in the medium dosage group computing the reduction from baseline to the dose maintenance phase (P<0.05). There were statistically more significant reductions in the duration and intensity of clonic signs in the medium dosage group (P<0.05). CONCLUSION: TPM has an early dose-dependant effect on secondarily GTCS in patients with pharmacoresistant partial seizures. SHORT COMMUNICATION: The present study intensively analyzed the duration, intensity, and frequency of secondarily generalized tonic and clonic signs in patients with pharmacoresistant partial seizures. The quantitative data suggested that TPM had a robust early inhibitory effect on secondarily generalized tonic-clonic signs; effects were more prominent in the medium dosage group (200 mg daily) than in the low dosage group (100 mg daily).
机译:目的:对托吡酯(TPM)治疗期间具有药物抗药性部分性发作的继发性全身性阵挛性阵挛性发作(GTCS)的持续时间,强度和频率进行强化和定量评估。方法:将30例继发GTCS的难治性部分性癫痫发作患者接受术前评估,随机分为低剂量(每天100 mg)和平行中等剂量(每天200 mg)TPM加药组(每组15例) 。研究阶段包括3天基线视频EEG阶段,10天TPM滴定阶段(不带视频EEG)和3天TPM剂量维持阶段(带EEG视频)。在基线和剂量维持阶段,使用视频-EEG监测记录癫痫发作,并针对每次记录的第二次一般性强直和阵挛症状测量以下参数:持续时间(持续秒),强度(0-3级),频率(每24小时内的数字)。结果:在基线阶段共进行了46例次发性强直-阵挛性症状的复杂部分性发作,在剂量维持阶段共进行了20次。在剂量维持阶段中,中剂量组的患者比低剂量组的患者第二次无GTCS(9对2,P <0.05)。组间比较表明,中等剂量组所有补品体征的持续时间减少更多,计算出从基线到剂量维持期的减少量(P <0.05)。在中等剂量组中,阵挛症状的持续时间和强度的减少在统计学上更为显着(P <0.05)。结论:TPM对部分耐药性癫痫患者的GTCS具有早期剂量依赖性作用。短期通讯:本研究集中分析了部分耐药性癫痫患者的继发性强直和阵挛性体征的持续时间,强度和频率。定量数据表明,TPM对继发性强直-阵挛征具有强烈的早期抑制作用。中剂量组(每天200 mg)的效果比低剂量组(每天100 mg)更显着。

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