German Center for Vertigo and Balance Disorders, Campus Großhadern, Munich University Hospital, Marchioninistrasse 15, 81377, Munich, Germany.
Department of Neurology, Munich University Hospital, Munich, Germany.
J Neurol. 2018 Feb;265(2):291-298. doi: 10.1007/s00415-017-8682-x. Epub 2017 Nov 27.
Vestibular paroxysmia (VP) is characterized by short, often oligosymptomatic attacks of vertigo which occur spontaneously or are sometimes provoked by turning the head. Despite the description of the disease almost 40 years ago (first termed "disabling positional vertigo"), no controlled treatment trial has been published to date. The Vestparoxy trial was designed as a randomized, placebo-controlled, double-blind cross-over trial to examine the therapeutic effect of oxcarbazepine (OXA) in patients with definite or probable VP.
Patients were recruited from August 2005 to December 2011 in the outpatient Dizziness Unit of the Department of Neurology of the Munich University Hospital, and randomized to receive OXA (first week: 300 mg once per day, second week: 300 mg b.i.d., third week: 300 mg t.i.d. until the end of the third month), followed by placebo or vice versa with a 1-month wash-out period in between. The primary endpoint was the number of days with one or more attacks. Secondary endpoints were the number of attacks during the observed days, and the median (for each day) duration of attacks. All these endpoints were assessed using standardized diaries collected at the end of each treatment phase.
Forty-three patients were randomized, 18 patients provided usable data (2525 patient days) for at least one treatment phase and were included in the main (intention-to-treat) analysis. The most common reasons for discontinuation documented were adverse events. The risk of experiencing a day with at least one attack was 0.41 under OXA, and 0.62 under placebo treatment, yielding a relative risk of 0.67 (95% CI 0.47-0.95, p = 0.025). The number of attacks during the observed days ratio was 0.53 (95% CI 0.42-0.68, p < 0.001) under OXA compared to placebo. Median attack duration was 4 s (Q25: 2 s, Q75: 120 s) under OXA, and 3 s (Q25: 2 s, Q75: 60 s) under placebo treatment. When days with no attacks, i.e., duration = 0, were included in the analysis, these figures changed to 0 (Q25: 0, Q75: 3 s), and 2 (Q25: 0, Q75: 6 s). No serious adverse events or new safety findings were identified during the trial.
The Vestparoxy trial showed a significant reduction of VP attacks under OXA compared to placebo treatment, confirming the known and revealing no new side effects.
前庭阵发性疾病(VP)的特征是短暂的、经常是症状单一的眩晕发作,这些发作是自发的,或者有时是转头引起的。尽管这种疾病在近 40 年前就已经被描述(最初被称为“致残性位置性眩晕”),但迄今为止,尚无对照治疗试验公布。Vestparoxy 试验被设计为一项随机、安慰剂对照、双盲交叉试验,以研究奥卡西平(OXA)在明确或可能的 VP 患者中的治疗效果。
2005 年 8 月至 2011 年 12 月期间,在慕尼黑大学医院神经科门诊眩晕科招募了患者,并随机接受 OXA 治疗(第 1 周:每天 300mg 一次,第 2 周:每天 300mg 两次,第 3 周:每天 300mg 三次,直到第三个月结束),然后是安慰剂或反之亦然,两者之间有 1 个月的洗脱期。主要终点是每天有一次或多次发作的天数。次要终点是观察期间的发作次数,以及每次发作的中位数(每天)持续时间。所有这些终点都使用每个治疗阶段结束时收集的标准化日记进行评估。
共有 43 名患者被随机分配,18 名患者提供了至少一个治疗阶段的可用数据(2525 个患者日),并被纳入主要(意向治疗)分析。记录的最常见停药原因是不良事件。在 OXA 治疗下,至少有一天发作的风险为 0.41,而在安慰剂治疗下为 0.62,相对风险为 0.67(95%CI 0.47-0.95,p=0.025)。与安慰剂相比,在观察期间,OXA 组的发作次数比为 0.53(95%CI 0.42-0.68,p<0.001)。OXA 组的中位发作持续时间为 4 秒(Q25:2 秒,Q75:120 秒),安慰剂组为 3 秒(Q25:2 秒,Q75:60 秒)。当包括无发作天数(即持续时间=0)时,这些数字分别变为 0(Q25:0,Q75:3 秒)和 2(Q25:0,Q75:6 秒)。试验期间未发现严重不良事件或新的安全发现。
Vestparoxy 试验显示,与安慰剂相比,奥卡西平治疗可显著减少 VP 发作,证实了已知的疗效,且未发现新的副作用。
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