特发性肺纤维化患者用力肺活量急性加重和下降与死亡率升高相关。
Acute Exacerbation and Decline in Forced Vital Capacity Are Associated with Increased Mortality in Idiopathic Pulmonary Fibrosis.
机构信息
1 Division of Pulmonary, Allergy, and Rheumatology Products, Office of New Drugs, Center for Drug Evaluation and Research, U.S. Food and Drug Administration, Silver Spring, Maryland; and.
2 Division of Pharmacometrics, Office of Clinical Pharmacology, Office of Translational Sciences, Center for Drug Evaluation and Research, U.S. Food and Drug Administration, Silver Spring, Maryland.
出版信息
Ann Am Thorac Soc. 2017 Sep;14(9):1395-1402. doi: 10.1513/AnnalsATS.201606-458OC.
RATIONALE
Exploration of FVC as it relates to mortality in idiopathic pulmonary fibrosis (IPF), a chronic, progressive, and ultimately fatal parenchymal lung disease, is important both clinically and to the current drug development paradigm. We evaluated the association between FVC decline and mortality in what is to our knowledge the largest well-characterized placebo cohort to date. Additionally, we sought to explore the risk of death caused by acute exacerbations and to further validate previously identified baseline predictors of mortality.
OBJECTIVES
To validate and further characterize FVC decline, acute exacerbations, and previously identified baseline predictors as they relate to risk of death.
METHODS
A total of 1,132 placebo subjects from six studies used for the clinical development of nintedanib and pirfenidone for the treatment of IPF were included in the present analysis. Deaths were captured as all-cause mortality. A stratified Cox proportional hazards model was used to test the association between baseline predictors, decline in FVC % predicted from baseline, acute exacerbations, and death. Decline in FVC % predicted and exacerbations were treated as time-varying covariates.
RESULTS
Subjects were followed for a mean of 60 weeks. At baseline, age, smoking status, lower FVC % predicted, and lower diffusing capacity of the lung for carbon monoxide % predicted were associated with an increased risk of death. The risk of death was also increased for subjects having one or more exacerbations with a hazard ratio (HR) of 10.3 (95% confidence interval [CI], 5.7-18.7). Compared with an FVC % predicted absolute decline from baseline at any time during the study of less than 5%, a decline greater than or equal to 10% to less than 15% was associated with an increased risk of death, with an HR of 2.2 (95% CI, 1.1-4.4), as was a decline greater than or equal to 15%, which was estimated with an HR of 6.1 (95% CI, 3.1-11.8). A decline ranging from greater than or equal to 5% to less than 10% was not associated with increased mortality.
CONCLUSIONS
Our analyses validate the importance of baseline FVC, diffusing capacity of the lung for carbon monoxide, age, and smoking status as predictors of mortality and strengthen the association between decline in FVC and exacerbations with death, verifying a decline in FVC as an appropriate endpoint in IPF drug development. Clinical trial registered with www.clinicaltrials.gov (NCT00514683, NCT01335464, NCT01335477, NCT00287729, NCT00287716, and NCT01366209).
背景
特发性肺纤维化(IPF)是一种慢性、进行性、最终致命的肺实质疾病,探索用力肺活量(FVC)与死亡率之间的关系在临床上和当前药物开发范式中都很重要。我们评估了在迄今为止最大的特征良好的安慰剂队列中,FVC 下降与死亡率之间的关联。此外,我们试图探索急性加重引起的死亡风险,并进一步验证先前确定的死亡率预测基线因素。
目的
验证并进一步描述 FVC 下降、急性加重和先前确定的基线预测因素与死亡风险的关系。
方法
本分析纳入了来自 6 项用于尼达尼布和吡非尼酮治疗 IPF 的临床开发研究的 1132 名安慰剂受试者。死亡被记录为全因死亡率。使用分层 Cox 比例风险模型来检验基线预测因素、从基线预测的 FVC 百分比下降、急性加重与死亡之间的关联。FVC 预测百分比下降和加重被视为随时间变化的协变量。
结果
受试者的平均随访时间为 60 周。基线时,年龄、吸烟状况、较低的 FVC 预测百分比和较低的一氧化碳弥散量预测百分比与死亡风险增加相关。有一次或多次加重的受试者死亡风险也增加,风险比(HR)为 10.3(95%置信区间[CI],5.7-18.7)。与研究期间任何时候 FVC 预测百分比的绝对下降小于 5%相比,下降大于或等于 10%至小于 15%与死亡风险增加相关,HR 为 2.2(95%CI,1.1-4.4),下降大于或等于 15%也与死亡风险增加相关,HR 为 6.1(95%CI,3.1-11.8)。FVC 预测百分比下降从大于或等于 5%至小于 10%与死亡率增加无关。
结论
我们的分析验证了基线 FVC、一氧化碳弥散量、年龄和吸烟状况作为死亡率预测因素的重要性,并加强了 FVC 下降与急性加重与死亡之间的关联,验证了 FVC 下降作为 IPF 药物开发中合适的终点。临床试验在 www.clinicaltrials.gov 注册(NCT00514683、NCT01335464、NCT01335477、NCT00287729、NCT00287716 和 NCT01366209)。
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