为囊性纤维化肺部恶化治疗反应的前瞻性研究确定终点。
Rationalizing endpoints for prospective studies of pulmonary exacerbation treatment response in cystic fibrosis.
机构信息
Case Western Reserve University School of Medicine, Cleveland, OH 44106, USA.
University of Washington, Seattle, WA 98121, USA; CFF Therapeutics Development Network Coordinating Center, Seattle Children's Research Institute, Seattle, WA 98105, USA.
出版信息
J Cyst Fibros. 2017 Sep;16(5):607-615. doi: 10.1016/j.jcf.2017.04.004. Epub 2017 Apr 21.
BACKGROUND
Given the variability in pulmonary exacerbation (PEx) management within and between Cystic Fibrosis (CF) Care Centers, it is possible that some approaches may be superior to others. A challenge with comparing different PEx management approaches is lack of a community consensus with respect to treatment-response metrics. In this analysis, we assess the feasibility of using different response metrics in prospective randomized studies comparing PEx treatment protocols.
METHODS
Response parameters were compiled from the recent STOP (Standardized Treatment of PEx) feasibility study. Pulmonary function responses (recovery of best prior 6-month and 12-month FEV% predicted and absolute and relative FEV% predicted improvement from treatment initiation) and sign and symptom recovery from treatment initiation (measured by the Chronic Respiratory Infection Symptom Score [CRISS]) were studied as categorical and continuous variables. The proportion of patients retreated within 30days after the end of initial treatment was studied as a categorical variable. Sample sizes required to adequately power prospective 1:1 randomized superiority and non-inferiority studies employing candidate endpoints were explored.
RESULTS
The most sensitive endpoint was mean change in CRISS from treatment initiation, followed by mean absolute FEV% predicted change from initiation, with the two responses only modestly correlated (R=.157; P<0.0001). Recovery of previous best FEV was a problematic endpoint due to missing data and a substantial proportion of patients beginning PEx treatment with FEV exceeding their previous best measures (12.1% >12-month best, 19.6% >6-month best). Although mean outcome measures deteriorated approximately 2-weeks post-treatment follow-up, the effect was non-uniform: 62.7% of patients experienced an FEV worsening versus 49.0% who experienced a CRISS worsening.
CONCLUSIONS
Results from randomized prospective superiority and non-inferiority studies employing mean CRISS and FEV change from treatment initiation should prove compelling to the community. They will need to be large, but appear feasible.
背景
由于囊性纤维化(CF)护理中心内部和之间的肺部恶化(PEx)管理存在差异,因此某些方法可能优于其他方法。比较不同的 PEx 管理方法的一个挑战是缺乏针对治疗反应指标的社区共识。在这项分析中,我们评估了在比较 PEx 治疗方案的前瞻性随机研究中使用不同反应指标的可行性。
方法
从最近的 STOP(PEx 的标准化治疗)可行性研究中汇编了反应参数。使用慢性呼吸道感染症状评分(CRISS)作为分类和连续变量,研究了肺功能反应(最佳先前 6 个月和 12 个月 FEV%预测值的恢复以及从治疗开始的绝对和相对 FEV%预测值的改善)和从治疗开始的症状和体征恢复。在初始治疗结束后 30 天内再次治疗的患者比例作为分类变量进行研究。探讨了使用候选终点进行充分 1:1 随机优势和非劣效性研究所需的样本量。
结果
最敏感的终点是从治疗开始时 CRISS 的平均变化,其次是从起始时绝对 FEV%预测值的平均变化,这两个反应仅略有相关性(R=.157;P<0.0001)。由于数据缺失和大量开始 PEx 治疗的患者 FEV 超过其先前最佳测量值(12.1% > 12 个月最佳,19.6% > 6 个月最佳),因此先前最佳 FEV 的恢复是一个有问题的终点。尽管平均结果指标在治疗后随访约 2 周后恶化,但这种影响并不均匀:62.7%的患者出现 FEV 恶化,而 49.0%的患者出现 CRISS 恶化。
结论
采用从治疗开始时平均 CRISS 和 FEV 变化的随机前瞻性优势和非劣效性研究的结果应该对社区具有说服力。它们需要很大,但似乎是可行的。
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