TY - JOUR T1 - [Translated article] Deconstructing phenotypes in COPD: An analysis of the TRACE cohort JO - Archivos de Bronconeumología T2 - AU - Carrasco Hernández,Laura AU - Caballero Eraso,Candela AU - Ruiz-Duque,Borja AU - Abad Arranz,María AU - Márquez Martín,Eduardo AU - Calero Acuña,Carmen AU - Lopez-Campos,Jose Luis SN - 03002896 M3 - 10.1016/j.arbres.2020.12.039 DO - 10.1016/j.arbres.2020.12.039 UR - https://archbronconeumol.org/en-translated-article-deconstructing-phenotypes-in-articulo-S0300289621004075 AB - ObjectivesIn a clinical phenotype-based management strategy for COPD, it would be preferable to at least assign all patients to a phenotype, but to a single phenotype only. The aim of this study was to evaluate whether all patients are assigned to one and only one phenotype using the Spanish COPD guidelines (GesEPOC) 2017 and to evaluate the criteria that define these categories. MethodThe Time-based Register and Analysis of COPD Endpoints study (TRACE; clinicaltrials.gov NCT03485690) is a prospective cohort of COPD patients attending annual visits since 2012, which collects GesEPOC phenotypes. Although the GesEPOC recommends that patients considered to be at low risk are not phenotyped, an analysis of the criteria for identifying high- and low-risk phenotypes was performed, comparing the distribution of phenotypes and the criteria applied between these 2 groups. ResultsThe cohort included 970 patients with a confirmed diagnosis of COPD, divided into 427 (44.02%) low-risk and 543 (55.9%) high-risk patients. The most frequent phenotype was the non-exacerbator (44.9% of high-risk patients). Overall, 20.6% of low-risk patients met criteria for asthma-COPD overlap syndrome, while 9.2% of the cohort did not meet the diagnostic criteria for any phenotype, and 19.1% met the criteria for 2 phenotypes, with no differences between risk groups. ConclusionsOur data highlight some of the weaknesses of the current clinical phenotype strategy, revealing overlapping categories in some cases, and patients to whom no phenotype was assigned. ER -