首页> 外文期刊>Journal of neuro-oncology. >Oxcarbazepine monotherapy in patients with brain tumor-related epilepsy: Open-label pilot study for assessing the efficacy, tolerability and impact on quality of life
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Oxcarbazepine monotherapy in patients with brain tumor-related epilepsy: Open-label pilot study for assessing the efficacy, tolerability and impact on quality of life

机译:奥卡西平单药治疗脑肿瘤相关性癫痫患者:评估疗效,耐受性和对生活质量影响的开放性先导研究

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We conducted a prospective, observational study to verify the efficacy, tolerability and impact on quality of life, mood and global neurocognitive performances of oxcarbazepine monotherapy in patients with brain tumor-related epilepsy (BTRE). Patients were followed for 12 months. We recruited 25 patients (11 females 14 males; mean age 49.7) affected with BTRE (17 de novo patients and 7 in monotherapy with other antiepileptics) and introduced oxcarbazepine monotherapy because of uncontrolled seizures and/or side effects. At first visit, patients underwent neurological examination, Qolie 31P V2, EORTC QLQC30, Zung self-depression rating scale (ZSDRS) and adverse events profile. A seizure diary was given to each patient. Follow-up duration was 1-12 months (mean 7.1 months, 5 patients died and 10 dropped out). Totals of 16 patients underwent both chemotherapy and radiotherapy, 4 chemotherapy only, 1 radiotherapy only, and 4 did not undergo any systemic therapy. Mean dosage of oxcarbazepine was 1,230 mg/day (min 600, max 2,100 mg/ day). McNemar's test showed a significant difference in seizure freedom rate (P = 0.002) between baseline and final follow-up in the intent-to-treat population. Six patients (24%) had serious side effects and one patient (4%) mild. Logistic regression revealed that, in our study, chemotherapy and radiotherapy did not affect the efficacy of OXC in seizure outcome (P = 0.658). The test evaluation at final follow-up showed a significant improvement in ZSDRS (P = 0.011) and no change over time. Oxcarbazepine seems to be efficacious in controlling seizures and in improving mood in patients with BTRE, but special caution should be taken when it is administered during radiotherapy.
机译:我们进行了一项前瞻性观察研究,以验证奥卡西平单药治疗脑肿瘤相关性癫痫(BTRE)患者的疗效,耐受性以及对生活质量,情绪和整体神经认知功能的影响。随访患者12个月。我们招募了25例受BTRE感染的患者(11例女性,14例男性;平均年龄49.7)(其中17例是de novo患者,另外7例是与其他抗癫痫药一起接受单药治疗),并由于癫痫发作和/或不良反应引入了奥卡西平单药治疗。初次就诊时,患者接受了神经系统检查,Qolie 31P V2,EORTC QLQC30,Zung自我抑郁等级量表(ZSDRS)和不良事件概况。给每位患者提供癫痫日记。随访时间为1-12个月(平均7.1个月,死亡5例,退出10例)。共有16例患者同时接受了化学疗法和放射疗法,仅4例接受了化学疗法,仅1例接受了放射疗法,而4例未接受任何全身性治疗。奥卡西平的平均剂量为1,230 mg /天(最小600,最大2,100 mg /天)。 McNemar的测试显示,在意向性治疗人群中,基线和最终随访之间的癫痫发作自由率存在显着差异(P = 0.002)。 6例(24%)有严重的副作用,1例(4%)轻度。 Logistic回归显示,在我们的研究中,化学疗法和放射疗法不影响OXC在癫痫发作结果中的功效(P = 0.658)。最终随访中的测试评估显示ZSDRS有显着改善(P = 0.011),并且没有随时间变化。奥卡西平似乎在控制癫痫发作和改善BTRE患者的情绪方面是有效的,但是在放疗期间使用奥卡西平时应特别注意。

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