Clinic of Child Neuropsychiatry, Second University of Naples, Naples, Italy.
Seizure. 2010 Nov;19(9):587-91. doi: 10.1016/j.seizure.2010.09.008.
This is the first multicenter Italian experience with rufinamide as an adjunctive drug in children, adolescents and adults with Lennox-Gastaut syndrome. The patients were enrolled in a prospective, add-on, open-label treatment study from 11 Italian centers for children and adolescent epilepsy care. Forty-three patients (26 males, 17 females), aged between 4 and 34 years (mean 15.9 ± 7.3, median 15.0), were treated with rufinamide for a mean period of 12.3 months (range 3-21 months). Twenty patients were diagnosed as cryptogenic and 23 as symptomatic. Rufinamide was added to the baseline therapy at the starting dose of 10mg/kg body weight, evenly divided in two daily doses and then increased by 10mg/kg approximately every 3 days up to a maximum of 1000 mg/day in children aged ≥4 years with a body weight less than 30 kg. In patients more than 30 kg body weight, rufinamide could be titrated up to 3200 mg/day. After a mean follow-up period of 12.3 months (range 3-21 months), the final mean dose of rufinamide was 33.5mg/kg/24h (range 11.5-60) if combined to valproic acid, and of 54.5mg/kg/24h (range 21.8-85.6) without valproic acid. The response rate (≥50% decrease in countable seizures) was 60.5% (26 of 45 patients) in total; 51.1% experienced a 50-99% reduction in seizure frequency and complete seizure control was achieved in the last 4 weeks follow-up by 9.3% of patients. Two patients (4.7%) had a 25-50% seizure reduction, while seizure frequency remained unchanged in 13 (30.2%) and increased in 2 (4.7%). Reliable data for atypical absence seizures and myoclonic seizures were not available, as these are usually impossible to count. Ten patients (23.2%) reported adverse side effects, while taking rufinamide. They were generally mild and transient and most frequently included vomiting, drowsiness, irritability and loss of appetite. In conclusion, rufinamide as an adjunctive therapy reduced the number of drop attacks and major motor seizures in about 60% of patients with Lennox-Gastaut syndrome and produced only mild or moderate adverse side effects.
这是意大利首次在 Lennox-Gastaut 综合征的儿童、青少年和成人中使用鲁非酰胺作为辅助药物的多中心经验。患者从 11 个意大利儿童和青少年癫痫治疗中心参加了一项前瞻性、附加的、开放标签的治疗研究。43 名患者(26 名男性,17 名女性),年龄在 4 至 34 岁之间(平均 15.9±7.3,中位数 15.0),平均接受鲁非酰胺治疗 12.3 个月(范围 3-21 个月)。20 名患者被诊断为隐源性,23 名患者为症状性。鲁非酰胺以 10mg/kg 体重的起始剂量添加到基线治疗中,每天分为两次等分剂量,然后每 3 天增加 10mg/kg,最大剂量为 1000mg/天,适用于年龄≥4 岁且体重小于 30kg 的儿童。对于体重超过 30kg 的患者,鲁非酰胺的剂量可滴定至 3200mg/天。在平均 12.3 个月(范围 3-21 个月)的随访后,最终的鲁非酰胺平均剂量为 33.5mg/kg/24h(范围 11.5-60),如果与丙戊酸钠联合使用;而无丙戊酸钠时,平均剂量为 54.5mg/kg/24h(范围 21.8-85.6)。总共有 60.5%(45 名患者中的 26 名)的患者出现了反应(发作次数减少≥50%);51.1%的患者发作频率减少 50-99%,9.3%的患者在最后 4 周的随访中完全控制了发作。2 名患者(4.7%)发作减少 25-50%,而 13 名患者(30.2%)发作频率无变化,2 名患者(4.7%)发作频率增加。由于这些发作通常无法计数,因此无法获得关于非典型失神发作和肌阵挛发作的可靠数据。10 名患者(23.2%)在服用鲁非酰胺时出现不良反应。这些不良反应通常是轻微和短暂的,最常见的是呕吐、嗜睡、烦躁和食欲不振。总之,鲁非酰胺作为辅助治疗,使大约 60%的 Lennox-Gastaut 综合征患者的跌倒发作和主要运动性发作次数减少,并且只产生轻微或中度的不良反应。
Zotero 插件