4.7 Article

Subtyping COPD by Using Visual and Quantitative CT Imaging Features

期刊

CHEST
卷 157, 期 1, 页码 47-60

出版社

ELSEVIER
DOI: 10.1016/j.chest.2019.06.015

关键词

COPD; CT imaging; epidemiology; heterogeneity; subtype

资金

  1. National Institutes of Health [K08HL136928, P01 HL114501]
  2. Parker B. Francis Research Opportunity Award
  3. National Heart, Lung, and Blood Institute of the National Institutes of Health [U01 HL089897, U01 HL089856]
  4. COPD Foundation
  5. AstraZeneca
  6. Boehringer Ingelheim
  7. GlaxoSmithKline
  8. Novartis
  9. Pfizer
  10. Siemens
  11. Sunovion Pharmaceuticals

向作者/读者索取更多资源

BACKGROUND: Multiple studies have identified COPD subtypes by using visual or quantitative evaluation of CT images. However, there has been no systematic assessment of a combined visual and quantitative CT imaging classification. We integrated visually defined patterns of emphysema with quantitative imaging features and spirometry data to produce a set of 10 nonoverlapping CT imaging subtypes, and we assessed differences between subtypes in demographic features, physiological characteristics, longitudinal disease progression, and mortality. METHODS: We evaluated 9,080 current and former smokers in the COPDGene study who had available volumetric inspiratory and expiratory CT images obtained using a standardized imaging protocol. We defined 10 discrete, nonoverlapping CT imaging subtypes: no CT imaging abnormality, paraseptal emphysema (PSE), bronchial disease, small airway disease, mild emphysema, upper lobe predominant centrilobular emphysema (CLE), lower lobe predominant CLE, diffuse CLE, visual without quantitative emphysema, and quantitative without visual emphysema. Baseline and 5-year longitudinal characteristics and mortality were compared across these CT imaging subtypes. RESULTS: The overall mortality differed significantly between groups (P < .01) and was highest in the 3 moderate to severe CLE groups. Subjects having quantitative but not visual emphysema and subjects with visual but not quantitative emphysema were unique groups with mild COPD, at risk for progression, and with likely different underlying mechanisms. Subjects with PSE and/or moderate to severe CLE had substantial progression of emphysema over 5 years compared with findings in subjects with no CT imaging abnormality (P < .01). CONCLUSIONS: The combination of visual and quantitative CT imaging features reflects different underlying pathological processes in the heterogeneous COPD syndrome and provides a useful approach to reclassify types of COPD.

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