Epilepsy Center, Cleveland Neurological Institute, Cleveland Clinic, Cleveland, OH, USA.
Pediatric Neurology, University Hospitals Bristol and Weston, Bristol, UK.
Lancet Neurol. 2022 May;21(5):417-427. doi: 10.1016/S1474-4422(22)00077-1.
CDKL5 deficiency disorder (CDD) is a rare, X-linked, developmental and epileptic encephalopathy characterised by severe global developmental impairment and seizures that can begin in the first few months after birth and are often treatment refractory. Ganaxolone, an investigational neuroactive steroid, reduced seizure frequency in an open-label, phase 2 trial that included patients with CDD. We aimed to further assess the efficacy and safety of ganaxolone in patients with CDD-associated refractory epilepsy.
In the double-blind phase of this randomised, placebo-controlled, phase 3 trial, done at 39 outpatient clinics in eight countries (Australia, France, Israel, Italy, Poland, Russia, the UK, and the USA), patients were eligible if they were aged 2-21 years with a pathogenic or probably pathogenic CDKL5 variant and at least 16 major motor seizures (defined as bilateral tonic, generalised tonic-clonic, bilateral clonic, atonic, or focal to bilateral tonic-clonic) per 28 days in each 4-week period of an 8-week historical period. After a 6-week prospective baseline period, patients were randomly assigned (1:1) via an interactive web response system to receive either enteral adjunctive ganaxolone or matching enteral adjunctive placebo (maximum dose 63 mg/kg per day for patients weighing ≤28 kg or 1800 mg/day for patients weighing >28 kg) for 17 weeks. Patients, caregivers, investigators (including those analysing data), trial staff, and the sponsor (other than the investigational product manager) were masked to treatment allocation. The primary efficacy endpoint was percentage change in median 28-day major motor seizure frequency from the baseline period to the 17-week double-blind phase and was analysed (using a Wilcoxon-rank sum test) in all patients who received at least one dose of trial treatment and for whom baseline data were available. Safety (compared descriptively across groups) was analysed in all patients who received at least one dose of trial treatment. This study is registered with ClinicalTrials.gov, NCT03572933, and the open-label extension phase is ongoing.
Between June 25, 2018, and July 2, 2020, 114 patients were screened for eligibility, of whom 101 (median age 6 years [IQR 3 to 10]) were randomly assigned to receive either ganaxolone (n=50) or placebo (n=51). All patients received at least one dose of a study drug, but seizure frequency for one patient in the ganaxolone group was not recorded at baseline and so the primary endpoint was analysed in a population of 100 patients. There was a median percentage change in 28-day major motor seizure frequency of -30·7% (IQR -49·5 to -1·9) in the ganaxolone group and of -6·9% (-24·1 to 39·7) in the placebo group (p=0·0036). The Hodges-Lehmann estimate of median difference in responses to ganaxolone versus placebo was -27·1% (95% CI -47·9 to - 9·6). Treatment-emergent adverse events occurred in 43 (86%) of 50 patients in the ganaxolone group and in 45 (88%) of 51 patients in the placebo group. Somnolence, pyrexia, and upper respiratory tract infections occurred in at least 10% of patients in the ganaxolone group and more frequently than in the placebo group. Serious adverse events occurred in six (12%) patients in the ganaxolone group and in five (10%) patients in the placebo group. Two (4%) patients in the ganaxolone group and four (8%) patients in the placebo group discontinued the trial. There were no deaths in the double-blind phase.
Ganaxolone significantly reduced the frequency of CDD-associated seizures compared with placebo and was generally well tolerated. Results from what is, to our knowledge, the first controlled trial in CDD suggest a potential treatment benefit for ganaxolone. Long-term treatment is being assessed in the ongoing open-label extension phase of this trial.
Marinus Pharmaceuticals.
CDKL5 缺乏症(CDD)是一种罕见的 X 连锁发育性和癫痫性脑病,其特征为严重的全面发育障碍和癫痫发作,这些发作可能在出生后几个月内开始,且通常对治疗有抗性。加那洛酮是一种研究中的神经活性甾体,在包括 CDD 患者在内的开放标签、2 期试验中,降低了癫痫发作的频率。我们旨在进一步评估加那洛酮在 CDD 相关难治性癫痫患者中的疗效和安全性。
在这项在 8 个国家(澳大利亚、法国、以色列、意大利、波兰、俄罗斯、英国和美国)的 39 家门诊诊所进行的随机、安慰剂对照、3 期试验的双盲阶段中,符合条件的患者为年龄在 2-21 岁之间,携带致病性或可能致病性的 CDKL5 变异体,且在每个 8 周历史期的 4 周期间,至少有 16 次主要运动性癫痫发作(定义为双侧强直、全面强直阵挛、双侧阵挛、失神或局灶性至双侧强直阵挛)。在 6 周前瞻性基线期后,患者通过交互式网络响应系统以 1:1 的比例随机分配接受肠内辅助加那洛酮或匹配的肠内辅助安慰剂(对于体重≤28kg 的患者,最大剂量为 63mg/kg/天,对于体重>28kg 的患者,最大剂量为 1800mg/天),治疗 17 周。患者、照顾者、研究者(包括分析数据的研究者)、试验工作人员和赞助商(除了研究产品经理)对治疗分配均设盲。主要疗效终点是从基线期到 17 周双盲期的 28 天主要运动性癫痫发作频率的中位数变化百分比,在至少接受一次试验治疗且有基线数据的所有患者中进行分析(使用 Wilcoxon-rank sum 检验)。安全性(根据组间描述性比较)在至少接受一次试验治疗的所有患者中进行分析。这项研究在 ClinicalTrials.gov 上注册,NCT03572933,开放标签扩展阶段正在进行中。
在 2018 年 6 月 25 日至 2020 年 7 月 2 日期间,有 114 名患者接受了入选资格筛查,其中 101 名(中位年龄 6 岁[IQR 3-10])被随机分配接受加那洛酮(n=50)或安慰剂(n=51)。所有患者均至少接受了一次研究药物治疗,但加那洛酮组有 1 名患者的癫痫发作频率在基线期未记录,因此主要终点分析的人群为 100 名患者。加那洛酮组 28 天主要运动性癫痫发作频率的中位数变化百分比为-30.7%(IQR-49.5 至-1.9),安慰剂组为-6.9%(-24.1 至 39.7)(p=0.0036)。加那洛酮与安慰剂相比的反应中位数差异的 Hodges-Lehmann 估计值为-27.1%(95%CI-47.9 至-9.6)。在加那洛酮组中,50 名患者中有 43 名(86%)和安慰剂组中 51 名患者中有 45 名(88%)发生了治疗相关不良事件。在加那洛酮组中,至少有 10%的患者出现了嗜睡、发热和上呼吸道感染等不良事件,且比安慰剂组更为频繁。在加那洛酮组中,有 6 名(12%)患者和安慰剂组中 5 名(10%)患者发生了严重不良事件。有 2 名(4%)加那洛酮组患者和 4 名(8%)安慰剂组患者退出了试验。在双盲期没有死亡。
与安慰剂相比,加那洛酮显著降低了 CDD 相关癫痫发作的频率,且通常耐受性良好。我们所知,这是第一项在 CDD 中进行的对照试验,结果表明加那洛酮可能具有治疗益处。目前正在对该试验的开放标签扩展阶段进行长期治疗评估。
Marinus Pharmaceuticals。
