Leist T, Cook S, Comi G, Montalban X, Giovannoni G, Nolting A, Damian D, Syed S, Galazka A
Division of Clinical Neuroimmunology, Jefferson University, Comprehensive MS Center, Philadelphia, PA, USA.
Rutgers, The State University of New Jersey, New Jersey Medical School, Newark, NJ, USA.
Mult Scler Relat Disord. 2020 Nov;46:102572. doi: 10.1016/j.msard.2020.102572. Epub 2020 Oct 8.
Long-term safety data are of particular interest for any newly approved treatment in multiple sclerosis such as cladribine tablets 10 mg (MAVENCLAD®; 3.5 mg/kg cumulative dose over 2 years, referred to as cladribine tablets 3.5 mg/kg), which is approved in Europe and the USA. Here we provide the final report on the integrated analysis of the safety profile of cladribine tablets 3.5 mg/kg from the clinical development program, including final data from the PREMIERE registry.
Safety data for cladribine tablets 3.5 mg/kg from three previously reported Phase III studies (CLARITY, CLARITY Extension and ORACLE-MS), as well as the prospective, observational PREMIERE registry (which ran from November 2009 to October 2018; consisting of patients who had participated in at least one of the Phase III trials) were combined to provide the Monotherapy Oral cohort. Serious adverse events (SAEs) and predefined SAEs of special interest were recorded. Observation-adjusted incidence rates per 100 patient-years (Adj-AE per 100 PY) were used to assess adverse events (AEs). Standardized incidence ratios for malignancies were calculated in relation to a matched GLOBOCAN reference population, and risk differences (cladribine tablets versus placebo) were estimated.
The Monotherapy Oral cohort comprised 923 patients who received cladribine tablets 3.5 mg/kg and 641 patients who received placebo. Overall, the reported number of SAEs was higher in the cladribine tablets 3.5 mg/kg group (133/923 [14.4%] patients with at least 1 SAE), versus the placebo group (68/641 [10.6%] patients with at least 1 SAE). Four patients in the cladribine tablets 3.5 mg/kg group had lymphopenia classified as a serious event (resulting in an Adj-AE of 0.10 per 100 PY) and 2 patients had serious herpes zoster (resulting in an Adj-AE of 0.05 per 100 PY). There were no cases in the corresponding placebo groups. There was no difference between the cladribine tablets 3.5 mg/kg group and placebo in the overall incidence of infections. However herpetic infection AEs occurred more frequently in the cladribine tablets 3.5 mg/kg group (driven primarily by herpes zoster, followed by oral herpes and herpes simplex). Overall, there was a numerical imbalance in malignancy incidence between cladribine tablets 3.5 mg/kg and placebo, with an Adj-AE of 0.26 and 0.12 per 100 PY, respectively; however the difference was not statistically significant. The rate of malignancies observed with cladribine tablets 3.5 mg/kg in the final integrated safety analysis was not different from the expected rate in the matched GLOBOCAN reference population (standardized incidence ratio, 0.88; 95% CI, 0.44-1.69).
Additional patient-years of observation do not significantly alter the conclusions of earlier interim analyses, and no new major safety findings were identified in this consolidated analysis of safety data of cladribine tablets 3.5 mg/kg monotherapy in patients with relapsing-remitting multiple sclerosis.
对于多发性硬化症的任何新批准治疗方法,如10毫克克拉屈滨片(MAVENCLAD®;2年内累积剂量为3.5毫克/千克,称为3.5毫克/千克克拉屈滨片),长期安全性数据尤为重要,该药物已在欧洲和美国获批。在此,我们提供了关于3.5毫克/千克克拉屈滨片安全性概况综合分析的最终报告,该分析来自临床开发项目,包括PREMIERE注册研究的最终数据。
将之前报道的三项III期研究(CLARITY、CLARITY扩展研究和ORACLE-MS)以及前瞻性观察性PREMIERE注册研究(从2009年11月至2018年10月;由至少参加过一项III期试验的患者组成)中3.5毫克/千克克拉屈滨片的安全性数据合并,组成单药口服队列。记录严重不良事件(SAE)和特别关注的预定义SAE。使用每100患者年的观察调整发病率(每100 PY的调整AE)来评估不良事件(AE)。计算与匹配的GLOBOCAN参考人群相关的恶性肿瘤标准化发病率,并估计风险差异(克拉屈滨片与安慰剂)。
单药口服队列包括923例接受3.5毫克/千克克拉屈滨片治疗的患者和641例接受安慰剂治疗的患者。总体而言,3.5毫克/千克克拉屈滨片组报告的SAE数量更高(133/923 [14.4%] 至少发生1次SAE的患者),而安慰剂组为(68/641 [10.6%] 至少发生1次SAE的患者)。3.5毫克/千克克拉屈滨片组有4例患者的淋巴细胞减少被分类为严重事件(导致每100 PY的调整AE为0.10),2例患者发生严重带状疱疹(导致每100 PY的调整AE为0.05)。相应的安慰剂组无病例。3.5毫克/千克克拉屈滨片组与安慰剂组在感染总体发病率上无差异。然而,疱疹感染AE在3.5毫克/千克克拉屈滨片组中更频繁发生(主要由带状疱疹驱动,其次是口腔疱疹和单纯疱疹)。总体而言,3.5毫克/千克克拉屈滨片与安慰剂在恶性肿瘤发病率上存在数值差异,每100 PY的调整AE分别为0.26和0.12;然而,差异无统计学意义。在最终的综合安全性分析中,3.5毫克/千克克拉屈滨片观察到的恶性肿瘤发生率与匹配的GLOBOCAN参考人群中的预期发生率无差异(标准化发病率,0.88;95% CI,0.44 - 1.69)。
额外的患者年观察并未显著改变早期中期分析的结论,并且在这项对复发缓解型多发性硬化症患者3.5毫克/千克克拉屈滨片单药治疗安全性数据的综合分析中未发现新的主要安全性发现。
