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首页> 外文期刊>Seizure: the journal of the British Epilepsy Association >Topiramate monotherapy as broad-spectrum antiepileptic drug in a naturalistic clinical setting.
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Topiramate monotherapy as broad-spectrum antiepileptic drug in a naturalistic clinical setting.

机译:托吡酯单药作为广谱抗癫痫药在自然主义临床环境中使用。

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Topiramate was assessed in an open-label trial as broad-spectrum antiepileptic monotherapy, independently from the epilepsy type or syndrome. Adults and children aged 2 years and older, who were diagnosed with epilepsy within the last 5 years, treatment-naive or failing prior treatment with one antiepileptic drug (AED), received individually adjusted doses of topiramate, after escalation to 100mg/day over 4 weeks (maximum 400mg/day) or 3mg/kg/day over 6 weeks (maximum 9 mg/kg/day), respectively. Patients were followed for >or=7 months and optionally up to a maximum of 13 months. Data were analysed for all patients (n=692), as well as for focal (n=421) and generalized epilepsies (n=148). The median topiramate dose used was 125 mg/day in adults and 3.3mg/kg/day in children (or=50% reduction in mean monthly seizure frequency. Patients with focal and generalized epilepsiesalike responded to treatment (73.9 and 83.8% with at least 50% seizure reduction): 39.4% of patients with focal epilepsy and 61.5% of those with generalized epilepsy were seizure-free. The mean monthly seizure frequency was significantly reduced versus baseline at all visits (p<0.001). Similar response rates were obtained from the 237 patients completing the 1-year observation period. During the mandatory 7-month period of study, 8.8% of patients reported insufficient tolerability as a reason for dropout. The most frequent adverse event was paraesthesia. Our results support findings that emerge from controlled studies that topiramate is effective and well tolerated when used as initial or second monotherapy. They also suggest that in a naturalistic setting, overall good retention on treatment and seizure freedom are observed at low doses in a broad spectrum of epilepsies.
机译:托吡酯在一项开放试验中被评估为广谱抗癫痫单药治疗,独立于癫痫类型或综合征。在过去5年内被诊断出患有癫痫病且未进行过治疗或未使用一种抗癫痫药(AED)进行治疗而失败的2岁及2岁以上的成人和儿童,在4天内逐步升高剂量至100mg /天后,接受了单独调整的托吡酯剂量周(最大400毫克/天)或3毫克/千克/天,分别超过6周(最大9毫克/千克/天)。对患者进行了≥7个月的随访,并且可选地长达13个月。分析了所有患者(n = 692)以及局灶性(n = 421)和全身性癫痫(n = 148)的数据。成人使用托吡酯的中位剂量为125 mg /天,儿童(≤12岁)为3.3 mg / kg /天。总体而言,有80%的患者完成了为期7个月的研究。在此期间,无癫痫发作的比例为44.3%,而平均每月癫痫发作频率的降低比例为[>或= 50%],占76.3%。局灶性和全身性癫痫样患者对治疗有反应(73.9%和83.8%,癫痫发作减少至少50%):局灶性癫痫患者中39.4%和全身性癫痫患者中无癫痫发作为61.5%。与所有访视相比,平均每月癫痫发作频率均显着降低(p <0.001)。从完成1年观察期的237名患者中获得了相似的缓解率。在强制性的7个月研究期间,8.8%的患者报告耐受性不足是辍学的原因。最常见的不良事件是感觉异常。我们的结果支持从对照研究中得出的结果,托吡酯在用作初始或第二种单一疗法时有效且耐受性良好。他们还建议,在自然主义的环境中,在广泛的癫痫症中低剂量观察到总体上对治疗的良好保留和癫痫发作的自由。

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