Literature DB >> 24563194

Cluster analysis in the COPDGene study identifies subtypes of smokers with distinct patterns of airway disease and emphysema.

Peter J Castaldi1, Jennifer Dy, James Ross, Yale Chang, George R Washko, Douglas Curran-Everett, Andre Williams, David A Lynch, Barry J Make, James D Crapo, Russ P Bowler, Elizabeth A Regan, John E Hokanson, Greg L Kinney, Meilan K Han, Xavier Soler, Joseph W Ramsdell, R Graham Barr, Marilyn Foreman, Edwin van Beek, Richard Casaburi, Gerald J Criner, Sharon M Lutz, Steven I Rennard, Stephanie Santorico, Frank C Sciurba, Dawn L DeMeo, Craig P Hersh, Edwin K Silverman, Michael H Cho.   

Abstract

BACKGROUND: There is notable heterogeneity in the clinical presentation of patients with COPD. To characterise this heterogeneity, we sought to identify subgroups of smokers by applying cluster analysis to data from the COPDGene study.
METHODS: We applied a clustering method, k-means, to data from 10 192 smokers in the COPDGene study. After splitting the sample into a training and validation set, we evaluated three sets of input features across a range of k (user-specified number of clusters). Stable solutions were tested for association with four COPD-related measures and five genetic variants previously associated with COPD at genome-wide significance. The results were confirmed in the validation set.
FINDINGS: We identified four clusters that can be characterised as (1) relatively resistant smokers (ie, no/mild obstruction and minimal emphysema despite heavy smoking), (2) mild upper zone emphysema-predominant, (3) airway disease-predominant and (4) severe emphysema. All clusters are strongly associated with COPD-related clinical characteristics, including exacerbations and dyspnoea (p<0.001). We found strong genetic associations between the mild upper zone emphysema group and rs1980057 near HHIP, and between the severe emphysema group and rs8034191 in the chromosome 15q region (p<0.001). All significant associations were replicated at p<0.05 in the validation sample (12/12 associations with clinical measures and 2/2 genetic associations).
INTERPRETATION: Cluster analysis identifies four subgroups of smokers that show robust associations with clinical characteristics of COPD and known COPD-associated genetic variants.

Entities:  

Keywords:  COPD epidemiology; Emphysema

Mesh:

Year:  2014        PMID: 24563194      PMCID: PMC4004338          DOI: 10.1136/thoraxjnl-2013-203601

Source DB:  PubMed          Journal:  Thorax        ISSN: 0040-6376            Impact factor:   9.139


  25 in total

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5.  Sex differences in severe pulmonary emphysema.

Authors:  Fernando J Martinez; Jeffrey L Curtis; Frank Sciurba; Jeanette Mumford; Nicholas D Giardino; Gail Weinmann; Ella Kazerooni; Susan Murray; Gerard J Criner; Donald D Sin; James Hogg; Andrew L Ries; MeiLan Han; Alfred P Fishman; Barry Make; Eric A Hoffman; Zab Mohsenifar; Robert Wise
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6.  Airway wall thickening and emphysema show independent familial aggregation in chronic obstructive pulmonary disease.

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Authors:  Klaus F Rabe; Suzanne Hurd; Antonio Anzueto; Peter J Barnes; Sonia A Buist; Peter Calverley; Yoshinosuke Fukuchi; Christine Jenkins; Roberto Rodriguez-Roisin; Chris van Weel; Jan Zielinski
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10.  A genome-wide association study in chronic obstructive pulmonary disease (COPD): identification of two major susceptibility loci.

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  56 in total

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5.  NHLBI strategic visioning: setting an agenda together for the NHLBI of 2025.

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7.  Clean Fuels to Reduce Household Air Pollution and Improve Health. Still Hoping to Answer Why and How.

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8.  Quantitative Imaging Markers of Lung Function in a Smoking Population Distinguish COPD Subgroups with Differential Lung Cancer Risk.

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9.  Genome-Wide Association Study of the Genetic Determinants of Emphysema Distribution.

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Review 10.  Risk of Lung Disease in PI MZ Heterozygotes. Current Status and Future Research Directions.

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