Issam A Awad, Roberto J Alcazar-Felix, Agnieszka Stadnik, Serena Kinkade, Aditya Jhaveri, Justine Lee, Stephanie Hage, Javed Iqbal, Sean P Polster, Robert Shenkar, Kevin Treine, Nichol McBee, Noeleen Ostapkovich, Karen Lane, James K Liao, Matthew Sorrentino, Cornelia Lee, Kelly D Flemming, Romuald Girard, Timothy J Carroll, Daniel F Hanley
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Patients aged 18–80 years with untreated CCMs who had had symptomatic bleeding from a CCM lesion within the previous year were eligible. Patients were randomly allocated (1:1) to oral atorvastatin (80 mg daily for 2 years) or matching placebo. Investigators, clinical staff, and participants were masked to the assigned treatment. The primary efficacy outcome was the percentage change in mean lesional iron deposition per year, measured by quantitative susceptibility mapping (QSM) on MRI and averaged over 2 years; a decrease would signal potential benefit and an increase a safety concern. The primary efficacy outcome was analysed in the modified intention-to-treat cohort, including patients with at least one annual paired QSM assessment. Safety outcomes included rates of bleeds and serious adverse events necessitating drug discontinuation. This trial is registered at ClinicalTrials.gov (NCT02603328) and is completed.<h3>Findings</h3>Between July 25, 2018, and July 22, 2022, 326 patients were assessed for eligibility, and 80 patients were allocated either atorvastatin (n=41) or placebo (n=39). 29 (36%) patients were male and 51 (64%) were female. 64 (80%) patients (33 in the atorvastatin group and 31 in the placebo group) had at least one annual paired QSM assessment and were included in the modified intention-to-treat analyses. The mean annual percentage change in lesional QSM was 10·88 (SE 7·29) with atorvastatin versus 12·09 (SE 7·54) with placebo (treatment effect –1·22, 95% CI –22·25 to 19·81; p=0·91). Symptomatic haemorrhage was reported in six patients assigned atorvastatin and seven patients assigned placebo (relative risk 0·81, 95% CI 0·31 to 2·13). No patients had a serious adverse event requiring drug discontinuation and no deaths were recorded.<h3>Interpretation</h3>For people with symptomatic haemorrhage caused by CCMs, atorvastatin did not affect the mean change in lesional iron deposition on brain MRI over 2 years when compared with placebo. Atorvastatin was well tolerated and no safety concerns were noted. 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引用次数: 0
摘要
背景:脑海绵体畸形(CCMs)在症状性出血后再出血的风险很高,并伴有严重的临床后遗症。在动物模型中,阿托伐他汀被证明可以阻止CCM生长和出血。我们的目的是评估阿托伐他汀治疗CCMs患者症状性出血后再出血的安全性和有效性。方法:我们在芝加哥大学CCM卓越中心进行了1/2a期随机试验。年龄在18-80岁的未经治疗的CCM患者在前一年有CCM病变的症状性出血。患者被随机(1:1)分配到口服阿托伐他汀组(每天80mg,持续2年)或匹配的安慰剂组。调查人员、临床工作人员和参与者被蒙面接受指定的治疗。主要疗效指标是每年平均病变铁沉积的百分比变化,通过MRI定量敏感性制图(QSM)测量,平均超过2年;减少则意味着潜在的好处,同时增加了安全隐患。主要疗效结果在修改意向治疗队列中进行分析,包括至少进行一次年度配对QSM评估的患者。安全性指标包括出血率和需要停药的严重不良事件。该试验已在ClinicalTrials.gov注册(NCT02603328)并已完成。在2018年7月25日至2022年7月22日期间,对326例患者进行了资格评估,其中80例患者分配了阿托伐他汀(n=41)或安慰剂(n=39)。男性29例(36%),女性51例(64%)。64例(80%)患者(阿托伐他汀组33例,安慰剂组31例)至少进行了一次年度配对QSM评估,并被纳入改良意向治疗分析。阿托伐他汀组病变性QSM的年平均百分比变化为10.88 (SE 7.29),安慰剂组为12.09 (SE 7.54)(治疗效果- 1.22,95% CI - 22.25 ~ 19.81;p = 0·91)。6名患者接受阿托伐他汀治疗,7名患者接受安慰剂治疗(相对危险度0.81,95% CI 0.31 ~ 2.13)。没有患者发生需要停药的严重不良事件,也没有死亡记录。对于CCMs引起的症状性出血患者,与安慰剂相比,阿托伐他汀不影响2年内脑MRI上病变铁沉积的平均变化。阿托伐他汀耐受性良好,无安全性问题。该研究为罕见疾病的生物标志物驱动药物评估提供了一个有用的框架。资助美国国立卫生研究院。
Safety and efficacy of atorvastatin for rebleeding in cerebral cavernous malformations (AT CASH EPOC): a phase 1/2a, randomised placebo-controlled trial
Background
Cerebral cavernous malformations (CCMs) carry a high risk of rebleeding after symptomatic haemorrhage, with serious clinical sequelae. Atorvastatin was shown to prevent CCM growth and bleeding in animal models. We aimed to assess the safety and efficacy of atorvastatin on rebleeding in patients with CCMs after a symptomatic haemorrhage.
Methods
We did a phase 1/2a randomised trial at the University of Chicago's CCM Center of Excellence. Patients aged 18–80 years with untreated CCMs who had had symptomatic bleeding from a CCM lesion within the previous year were eligible. Patients were randomly allocated (1:1) to oral atorvastatin (80 mg daily for 2 years) or matching placebo. Investigators, clinical staff, and participants were masked to the assigned treatment. The primary efficacy outcome was the percentage change in mean lesional iron deposition per year, measured by quantitative susceptibility mapping (QSM) on MRI and averaged over 2 years; a decrease would signal potential benefit and an increase a safety concern. The primary efficacy outcome was analysed in the modified intention-to-treat cohort, including patients with at least one annual paired QSM assessment. Safety outcomes included rates of bleeds and serious adverse events necessitating drug discontinuation. This trial is registered at ClinicalTrials.gov (NCT02603328) and is completed.
Findings
Between July 25, 2018, and July 22, 2022, 326 patients were assessed for eligibility, and 80 patients were allocated either atorvastatin (n=41) or placebo (n=39). 29 (36%) patients were male and 51 (64%) were female. 64 (80%) patients (33 in the atorvastatin group and 31 in the placebo group) had at least one annual paired QSM assessment and were included in the modified intention-to-treat analyses. The mean annual percentage change in lesional QSM was 10·88 (SE 7·29) with atorvastatin versus 12·09 (SE 7·54) with placebo (treatment effect –1·22, 95% CI –22·25 to 19·81; p=0·91). Symptomatic haemorrhage was reported in six patients assigned atorvastatin and seven patients assigned placebo (relative risk 0·81, 95% CI 0·31 to 2·13). No patients had a serious adverse event requiring drug discontinuation and no deaths were recorded.
Interpretation
For people with symptomatic haemorrhage caused by CCMs, atorvastatin did not affect the mean change in lesional iron deposition on brain MRI over 2 years when compared with placebo. Atorvastatin was well tolerated and no safety concerns were noted. The study provides a useful framework for biomarker driven drug assessment in a rare disease.
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