SPIROMICS和COPDGene队列中预测病情加重的生物标志物
Biomarkers Predictive of Exacerbations in the SPIROMICS and COPDGene Cohorts.
作者信息
Keene Jason D, Jacobson Sean, Kechris Katerina, Kinney Gregory L, Foreman Marilyn G, Doerschuk Claire M, Make Barry J, Curtis Jeffrey L, Rennard Stephen I, Barr R Graham, Bleecker Eugene R, Kanner Richard E, Kleerup Eric C, Hansel Nadia N, Woodruff Prescott G, Han MeiLan K, Paine Robert, Martinez Fernando J, Bowler Russell P, O'Neal Wanda K
机构信息
1 University of Colorado Anschutz Medical Campus, Aurora, Colorado.
2 National Jewish Health, Denver, Colorado.
出版信息
Am J Respir Crit Care Med. 2017 Feb 15;195(4):473-481. doi: 10.1164/rccm.201607-1330OC.
RATIONALE
Chronic obstructive pulmonary disease exacerbations are associated with disease progression, higher healthcare cost, and increased mortality. Published predictors of future exacerbations include previous exacerbation, airflow obstruction, poor overall health, home oxygen use, and gastroesophageal reflux.
OBJECTIVES
To determine the value of adding blood biomarkers to clinical variables to predict exacerbations.
METHODS
Subjects from the SPIROMICS (Subpopulations and Intermediate Outcomes Measures in COPD Study) (n = 1,544) and COPDGene (Genetic Epidemiology of COPD) (n = 602) cohorts had 90 plasma or serum candidate proteins measured on study entry using Myriad-RBM multiplex panels. We defined total exacerbations as subject-reported worsening in respiratory health requiring therapy with corticosteroids and/or antibiotics, and severe exacerbations as those leading to hospitalizations or emergency room visits. We assessed retrospective exacerbations during the 12 months before enrollment and then documented prospective exacerbations in each cohort. Exacerbations were modeled for biomarker associations with negative binomial regression including clinical covariates (age, sex, percent predicted FEV, self-reported gastroesophageal reflux, St. George's Respiratory Questionnaire score, smoking status). We used the Stouffer-Liptak test to combine P values for metaanalysis.
MEASUREMENTS AND MAIN RESULTS
Between the two cohorts, 3,471 total exacerbations (1,044 severe) were reported. We identified biomarkers within each cohort that were significantly associated with a history of exacerbation and with a future exacerbation, but there was minimal replication between the cohorts. Although established clinical features were predictive of exacerbations, of the blood biomarkers only decorin and α-macroglobulin increased predictive value for future severe exacerbations.
CONCLUSIONS
Blood biomarkers were significantly associated with the occurrence of exacerbations but were not robust between cohorts and added little to the predictive value of clinical covariates for exacerbations.
原理
慢性阻塞性肺疾病急性加重与疾病进展、更高的医疗成本和死亡率增加相关。已公布的未来急性加重的预测因素包括既往急性加重、气流阻塞、整体健康状况差、家庭氧疗使用情况以及胃食管反流。
目的
确定在临床变量中加入血液生物标志物对预测急性加重的价值。
方法
来自SPIROMICS(慢性阻塞性肺疾病研究中的亚组和中间结局指标)队列(n = 1544)和COPDGene(慢性阻塞性肺疾病的遗传流行病学)队列(n = 602)的受试者在研究入组时使用Myriad-RBM多重检测板检测了90种血浆或血清候选蛋白。我们将总的急性加重定义为受试者报告的呼吸健康状况恶化,需要使用皮质类固醇和/或抗生素进行治疗,将严重急性加重定义为导致住院或急诊就诊的情况。我们评估了入组前12个月内的回顾性急性加重情况,然后记录每个队列中的前瞻性急性加重情况。使用负二项回归模型对急性加重与生物标志物的关联进行建模,包括临床协变量(年龄、性别、预测FEV百分比、自我报告的胃食管反流、圣乔治呼吸问卷评分、吸烟状况)。我们使用Stouffer-Liptak检验合并P值进行荟萃分析。
测量指标和主要结果
在两个队列中,共报告了3471次总的急性加重(1044次严重急性加重)。我们在每个队列中确定了与既往急性加重病史和未来急性加重显著相关的生物标志物,但队列之间的重复性极小。尽管既定的临床特征可预测急性加重,但在血液生物标志物中,只有核心蛋白聚糖和α-巨球蛋白增加了对未来严重急性加重的预测价值。
结论
血液生物标志物与急性加重的发生显著相关,但在队列之间并不稳定,对急性加重临床协变量的预测价值增加不大。
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