来自美国和英国囊性纤维化注册中心的数据支持 CFTR 调节剂 ivacaftor 对疾病的修饰作用。
Data from the US and UK cystic fibrosis registries support disease modification by CFTR modulation with ivacaftor.
机构信息
Vertex Pharmaceuticals Incorporated, Boston, Massachusetts, USA.
Vertex Pharmaceuticals (Europe) Limited, London, UK.
出版信息
Thorax. 2018 Aug;73(8):731-740. doi: 10.1136/thoraxjnl-2017-210394. Epub 2018 May 10.
BACKGROUND
Ivacaftor is the first cystic fibrosis transmembrane conductance regulator (CFTR) modulator demonstrating clinical benefit in patients with cystic fibrosis (CF). As ivacaftor is intended for chronic, lifelong use, understanding long-term effects is important for patients and healthcare providers.
OBJECTIVE
This ongoing, observational, postapproval safety study evaluates clinical outcomes and disease progression in ivacaftor-treated patients using data from the US and the UK CF registries following commercial availability.
METHODS
Annual analyses compare ivacaftor-treated and untreated matched comparator patients for: risks of death, transplantation, hospitalisation, pulmonary exacerbation; prevalence of CF-related complications and microorganisms and lung function changes in a subset of patients who initiated ivacaftor in the first year of commercial availability. Results from the 2014 analyses (2 and 3 years following commercial availability in the UK and USA, respectively) are presented here.
RESULTS
Analyses included 1256 ivacaftor-treated and 6200 comparator patients from the USA and 411 ivacaftor-treated and 2069 comparator patients from the UK. No new safety concerns were identified based on the evaluation of clinical outcomes included in the analyses. As part of safety evaluations, ivacaftor-treated US patients were observed to have significantly lower risks of death (0.6% vs 1.6%, p=0.0110), transplantation (0.2% vs 1.1%, p=0.0017), hospitalisation (27.5% vs 43.1%, p<0.0001) and pulmonary exacerbation (27.8% vs 43.3%, p<0.0001) relative to comparators; trends were similar in the UK. In both registries, ivacaftor-treated patients had a lower prevalence of CF-related complications and select microorganisms and had better preserved lung function.
CONCLUSIONS
While general limitations of observational research apply, analyses revealed favourable results for clinically important outcomes among ivacaftor-treated patients, adding to the growing body of literature supporting disease modification by CFTR modulation with ivacaftor.
EU PAS REGISTRATION NUMBER
EUPAS4270.
背景
依伐卡托是首个在囊性纤维化(CF)患者中显示临床获益的囊性纤维化跨膜电导调节因子(CFTR)调节剂。由于依伐卡托旨在用于慢性、终身使用,因此了解其长期影响对于患者和医疗保健提供者很重要。
目的
本项正在进行的、观察性的、上市后安全性研究使用美国和英国 CF 登记处的数据,评估了上市后依伐卡托治疗患者的临床结局和疾病进展。
方法
每年的分析将接受依伐卡托治疗和未接受治疗的匹配对照患者进行比较:死亡、移植、住院、肺部恶化的风险;CF 相关并发症和微生物的流行率,以及在上市后第一年开始接受依伐卡托治疗的患者的肺功能变化。这里呈现的是 2014 年分析的结果(分别在英国和美国上市后 2 年和 3 年)。
结果
分析纳入了来自美国的 1256 例依伐卡托治疗患者和 6200 例对照患者,以及来自英国的 411 例依伐卡托治疗患者和 2069 例对照患者。基于分析中包含的临床结局评估,没有发现新的安全性问题。作为安全性评估的一部分,观察到接受依伐卡托治疗的美国患者的死亡(0.6% 比 1.6%,p=0.0110)、移植(0.2% 比 1.1%,p=0.0017)、住院(27.5% 比 43.1%,p<0.0001)和肺部恶化(27.8% 比 43.3%,p<0.0001)风险显著低于对照患者;英国的趋势相似。在两个登记处,接受依伐卡托治疗的患者 CF 相关并发症和特定微生物的流行率较低,肺功能保存较好。
结论
尽管观察性研究存在一般局限性,但分析结果显示,依伐卡托治疗患者在重要临床结局方面有较好的结果,这为依伐卡托通过调节 CFTR 来改善疾病提供了更多的文献支持。
欧盟注册编号
EUPAS4270。
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