Subtypes of COPD have unique distributions and differential risk of mortality

Kendra A. Young; Elizabeth A. Regan; Mei Lan K. Han; Sharon M. Lutz; Margaret Ragland; Peter J. Castaldi; George R. Washko; Michael H. Cho; Mathew Strand; Douglas Curran-Everett; Terri H. Beaty; Russell P. Bowler; Emily S. Wan; David A. Lynch; Barry J. Make; Edwin K. Silverman; James D. Crapo; John E. Hokanson; Gregory L. Kinney

doi:10.15326/jcopdf.6.5.2019.0150

Subtypes of COPD have unique distributions and differential risk of mortality

Kendra A. Young, Elizabeth A. Regan, Mei Lan K. Han, Sharon M. Lutz, Margaret Ragland, Peter J. Castaldi, George R. Washko, Michael H. Cho, Mathew Strand, Douglas Curran-Everett, Terri H. Beaty, Russell P. Bowler, Emily S. Wan, David A. Lynch, Barry J. Make, Edwin K. Silverman, James D. Crapo, John E. Hokanson, Gregory L. Kinney

School of Medicine

Research output: Contribution to journal › Article › peer-review

10 Scopus citations

Abstract

Background: Previous attempts to explore the heterogeneity of chronic obstructive pulmonary disease (COPD) clustered individual patients using clinical, demographic, and disease features. We developed continuous multidimensional disease axes based on radiographic and spirometric variables that split into an airwaypredominant axis and an emphysema-predominant axis. Methods: The COPD Genetic Epidemiology study (COPDGene®) is a cohort of current and former smokers, > 45 years, with at least 10 pack years of smoking history. Spirometry measures, blood pressure and body mass were directly measured. Mortality was assessed through continuing longitudinal follow-up and cause of death was adjudicated. Among 8157 COPDGene® participants with complete spirometry and computed tomography (CT) measures, the top 2 deciles of the airway-predominant and emphysema-predominant axes previously identified were used to categorize individuals into 3 groups having the highest risk for mortality using Cox proportional hazard ratios. These groups were also assessed for causal mortality. Biomarkers of COPD (fibrinogen, soluble receptor for advanced glycation end products [sRAGE], C-reactive protein [CRP], clara cell secretory protein [CC16], surfactant-D [SP-D]) were compared by group. Findings: High-risk subtype classification was defined for 2638 COPDGene® participants who were in the highest 2 deciles of either the airway-predominant and/or emphysema-predominant axis (32% of the cohort). These high-risk participants fell into 3 groups: Airway-predominant disease only (APD-only), emphysemapredominant disease only (EPD-only) and combined APD-EPD. There was 26% mortality for the APD-only group, 21% mortality for the EPD-only group, and 54% mortality for the combined APD-EPD group. The APDonly group (n=1007) was younger, had a lower forced expiratory volume in 1 second (FEV1) percent (%) predicted and a strong association with the preserved ratio-impaired spirometry (PRISm) quadrant. The EPD-only group (n=1006) showed a relatively higher FEV1 % predicted and included largely GOLD stage 0, 1 and 2 partipants. Individuals in each of the 3 high-risk groups were at greater risk for respiratory mortality, while those in the APD-only group were additionally at greater risk for cardiovascular mortality. Biomarker analysis demonstrated a significant association of the APD-only group with CRP, and sRAGE demonstrated greatest significance with both the EPD-only and the combined APD-EPD groups. Interpretation: Among current and former smokers, individuals in the highest 2 deciles for mortality risk on the airway-predominant axis and the emphysema-predominant axis have unique associations to spirometric patterns, different imaging characteristics, biomarkers and causal mortality.

Original language	English (US)
Pages (from-to)	400-413
Number of pages	14
Journal	Chronic Obstructive Pulmonary Diseases
Volume	6
Issue number	5
DOIs	https://doi.org/10.15326/jcopdf.6.5.2019.0150
State	Published - 2019

Keywords

Airwaypredominant disease
Biomarkers
COPD
COPD Genetic Epidemiology
COPDGene®
Chronic obstructive pulmonary disease
Emphysema-predominant disease
Mortality
PRISm
Preserved ratio-impaired spirometry
Subtypes

ASJC Scopus subject areas

Pulmonary and Respiratory Medicine

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10.15326/jcopdf.6.5.2019.0150

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Young, K. A., Regan, E. A., Han, M. L. K., Lutz, S. M., Ragland, M., Castaldi, P. J., Washko, G. R., Cho, M. H., Strand, M., Curran-Everett, D., Beaty, T. H., Bowler, R. P., Wan, E. S., Lynch, D. A., Make, B. J., Silverman, E. K., Crapo, J. D., Hokanson, J. E., & Kinney, G. L. (2019). Subtypes of COPD have unique distributions and differential risk of mortality. Chronic Obstructive Pulmonary Diseases, 6(5), 400-413. https://doi.org/10.15326/jcopdf.6.5.2019.0150

Young, KA, Regan, EA, Han, MLK, Lutz, SM, Ragland, M, Castaldi, PJ, Washko, GR, Cho, MH, Strand, M, Curran-Everett, D, Beaty, TH, Bowler, RP, Wan, ES, Lynch, DA, Make, BJ, Silverman, EK, Crapo, JD, Hokanson, JE & Kinney, GL 2019, 'Subtypes of COPD have unique distributions and differential risk of mortality', Chronic Obstructive Pulmonary Diseases, vol. 6, no. 5, pp. 400-413. https://doi.org/10.15326/jcopdf.6.5.2019.0150

@article{cb34563a918d4df5a0e2853d8ebff902,

title = "Subtypes of COPD have unique distributions and differential risk of mortality",

abstract = "Background: Previous attempts to explore the heterogeneity of chronic obstructive pulmonary disease (COPD) clustered individual patients using clinical, demographic, and disease features. We developed continuous multidimensional disease axes based on radiographic and spirometric variables that split into an airwaypredominant axis and an emphysema-predominant axis. Methods: The COPD Genetic Epidemiology study (COPDGene{\textregistered}) is a cohort of current and former smokers, > 45 years, with at least 10 pack years of smoking history. Spirometry measures, blood pressure and body mass were directly measured. Mortality was assessed through continuing longitudinal follow-up and cause of death was adjudicated. Among 8157 COPDGene{\textregistered} participants with complete spirometry and computed tomography (CT) measures, the top 2 deciles of the airway-predominant and emphysema-predominant axes previously identified were used to categorize individuals into 3 groups having the highest risk for mortality using Cox proportional hazard ratios. These groups were also assessed for causal mortality. Biomarkers of COPD (fibrinogen, soluble receptor for advanced glycation end products [sRAGE], C-reactive protein [CRP], clara cell secretory protein [CC16], surfactant-D [SP-D]) were compared by group. Findings: High-risk subtype classification was defined for 2638 COPDGene{\textregistered} participants who were in the highest 2 deciles of either the airway-predominant and/or emphysema-predominant axis (32% of the cohort). These high-risk participants fell into 3 groups: Airway-predominant disease only (APD-only), emphysemapredominant disease only (EPD-only) and combined APD-EPD. There was 26% mortality for the APD-only group, 21% mortality for the EPD-only group, and 54% mortality for the combined APD-EPD group. The APDonly group (n=1007) was younger, had a lower forced expiratory volume in 1 second (FEV1) percent (%) predicted and a strong association with the preserved ratio-impaired spirometry (PRISm) quadrant. The EPD-only group (n=1006) showed a relatively higher FEV1 % predicted and included largely GOLD stage 0, 1 and 2 partipants. Individuals in each of the 3 high-risk groups were at greater risk for respiratory mortality, while those in the APD-only group were additionally at greater risk for cardiovascular mortality. Biomarker analysis demonstrated a significant association of the APD-only group with CRP, and sRAGE demonstrated greatest significance with both the EPD-only and the combined APD-EPD groups. Interpretation: Among current and former smokers, individuals in the highest 2 deciles for mortality risk on the airway-predominant axis and the emphysema-predominant axis have unique associations to spirometric patterns, different imaging characteristics, biomarkers and causal mortality.",

keywords = "Airwaypredominant disease, Biomarkers, COPD, COPD Genetic Epidemiology, COPDGene{\textregistered}, Chronic obstructive pulmonary disease, Emphysema-predominant disease, Mortality, PRISm, Preserved ratio-impaired spirometry, Subtypes",

author = "Young, {Kendra A.} and Regan, {Elizabeth A.} and Han, {Mei Lan K.} and Lutz, {Sharon M.} and Margaret Ragland and Castaldi, {Peter J.} and Washko, {George R.} and Cho, {Michael H.} and Mathew Strand and Douglas Curran-Everett and Beaty, {Terri H.} and Bowler, {Russell P.} and Wan, {Emily S.} and Lynch, {David A.} and Make, {Barry J.} and Silverman, {Edwin K.} and Crapo, {James D.} and Hokanson, {John E.} and Kinney, {Gregory L.}",

note = "Funding Information: Abbreviations: chronic obstructive pulmonary disease, COPD; COPD Genetic Epidemiology, COPDGene{\textregistered}; computed tomography, CT; C-reactive protein, CRP; surfactant-D, SP-D; airway-predeominant disease only, APD-only; empysema-preeominant disease only, EPD-only; combined airway-predominant disease and emphysema-predominant disease, APD-EPD; preserved ratio-impaired spirometry, PRISm; Body mass index-airway Obstruction-Dyspnea-Exercise capacity index, BODE; soluble receptor for advanced glycation end products, sRAGE; Global initiative for chronic Obstructive Lung Disease, GOLD; longintudinal follow-up, LFU; body mass index, BMI; cardiovascular disease, CVD; modified Medical Research Council, mMRC; Social Security Death Index, SSDI; wall area percentage, WA%; standard deviation, SD; hazard ratio, HR; confidence interval, CI; analysis of variance, ANOVA; low attenuation area percentage, LAA% Funding Support: COPDGene{\textregistered} is supported by the National Heart, Lung, and Blood Institute (U01 HL089897 and U01 HL089856). This work was also supported by National Heart, Lung and Blood Institute K01 HL125858 (SML). MHC was supported by NHLBI grants R01HL113264, R01HL137927, and R01HL135142. COPDGene{\textregistered} is also supported by the COPD Foundation through contributions made to an Industry Advisory Board comprised of AstraZeneca, Boehringer Ingelheim, GlaxoSmithKline, Novartis, Pfizer, Siemens and Sunovion. Date of Acceptance: October 28, 2019 Citation: Young KA, Regan EA, Han MK, et al and the COPDGene Investigators. Subtypes of COPD have unique distributions and differential risk of mortality. Chronic Obstr Pulm Dis. 2019;6(5):400-413. doi: https://doi.org/10.15326/jcopdf.6.5.2019.0150 Funding Information: MHC and EKS have received grant support from GlaxoSmithKline. RPB has received consulting fees from Boehringer Ingelheim, AstraZeneca, and GlaxoSmithKline. All other authors declare they have no conflicting interests. Publisher Copyright: {\textcopyright} AJCEM 2020.",

year = "2019",

doi = "10.15326/jcopdf.6.5.2019.0150",

language = "English (US)",

volume = "6",

pages = "400--413",

journal = "Chronic Obstructive Pulmonary Diseases",

issn = "2372-952X",

publisher = "COPD Foundation",

number = "5",

}

TY - JOUR

T1 - Subtypes of COPD have unique distributions and differential risk of mortality

AU - Young, Kendra A.

AU - Regan, Elizabeth A.

AU - Han, Mei Lan K.

AU - Lutz, Sharon M.

AU - Ragland, Margaret

AU - Castaldi, Peter J.

AU - Washko, George R.

AU - Cho, Michael H.

AU - Strand, Mathew

AU - Curran-Everett, Douglas

AU - Beaty, Terri H.

AU - Bowler, Russell P.

AU - Wan, Emily S.

AU - Lynch, David A.

AU - Make, Barry J.

AU - Silverman, Edwin K.

AU - Crapo, James D.

AU - Hokanson, John E.

AU - Kinney, Gregory L.

N1 - Funding Information: Abbreviations: chronic obstructive pulmonary disease, COPD; COPD Genetic Epidemiology, COPDGene®; computed tomography, CT; C-reactive protein, CRP; surfactant-D, SP-D; airway-predeominant disease only, APD-only; empysema-preeominant disease only, EPD-only; combined airway-predominant disease and emphysema-predominant disease, APD-EPD; preserved ratio-impaired spirometry, PRISm; Body mass index-airway Obstruction-Dyspnea-Exercise capacity index, BODE; soluble receptor for advanced glycation end products, sRAGE; Global initiative for chronic Obstructive Lung Disease, GOLD; longintudinal follow-up, LFU; body mass index, BMI; cardiovascular disease, CVD; modified Medical Research Council, mMRC; Social Security Death Index, SSDI; wall area percentage, WA%; standard deviation, SD; hazard ratio, HR; confidence interval, CI; analysis of variance, ANOVA; low attenuation area percentage, LAA% Funding Support: COPDGene® is supported by the National Heart, Lung, and Blood Institute (U01 HL089897 and U01 HL089856). This work was also supported by National Heart, Lung and Blood Institute K01 HL125858 (SML). MHC was supported by NHLBI grants R01HL113264, R01HL137927, and R01HL135142. COPDGene® is also supported by the COPD Foundation through contributions made to an Industry Advisory Board comprised of AstraZeneca, Boehringer Ingelheim, GlaxoSmithKline, Novartis, Pfizer, Siemens and Sunovion. Date of Acceptance: October 28, 2019 Citation: Young KA, Regan EA, Han MK, et al and the COPDGene Investigators. Subtypes of COPD have unique distributions and differential risk of mortality. Chronic Obstr Pulm Dis. 2019;6(5):400-413. doi: https://doi.org/10.15326/jcopdf.6.5.2019.0150 Funding Information: MHC and EKS have received grant support from GlaxoSmithKline. RPB has received consulting fees from Boehringer Ingelheim, AstraZeneca, and GlaxoSmithKline. All other authors declare they have no conflicting interests. Publisher Copyright: © AJCEM 2020.

PY - 2019

Y1 - 2019

N2 - Background: Previous attempts to explore the heterogeneity of chronic obstructive pulmonary disease (COPD) clustered individual patients using clinical, demographic, and disease features. We developed continuous multidimensional disease axes based on radiographic and spirometric variables that split into an airwaypredominant axis and an emphysema-predominant axis. Methods: The COPD Genetic Epidemiology study (COPDGene®) is a cohort of current and former smokers, > 45 years, with at least 10 pack years of smoking history. Spirometry measures, blood pressure and body mass were directly measured. Mortality was assessed through continuing longitudinal follow-up and cause of death was adjudicated. Among 8157 COPDGene® participants with complete spirometry and computed tomography (CT) measures, the top 2 deciles of the airway-predominant and emphysema-predominant axes previously identified were used to categorize individuals into 3 groups having the highest risk for mortality using Cox proportional hazard ratios. These groups were also assessed for causal mortality. Biomarkers of COPD (fibrinogen, soluble receptor for advanced glycation end products [sRAGE], C-reactive protein [CRP], clara cell secretory protein [CC16], surfactant-D [SP-D]) were compared by group. Findings: High-risk subtype classification was defined for 2638 COPDGene® participants who were in the highest 2 deciles of either the airway-predominant and/or emphysema-predominant axis (32% of the cohort). These high-risk participants fell into 3 groups: Airway-predominant disease only (APD-only), emphysemapredominant disease only (EPD-only) and combined APD-EPD. There was 26% mortality for the APD-only group, 21% mortality for the EPD-only group, and 54% mortality for the combined APD-EPD group. The APDonly group (n=1007) was younger, had a lower forced expiratory volume in 1 second (FEV1) percent (%) predicted and a strong association with the preserved ratio-impaired spirometry (PRISm) quadrant. The EPD-only group (n=1006) showed a relatively higher FEV1 % predicted and included largely GOLD stage 0, 1 and 2 partipants. Individuals in each of the 3 high-risk groups were at greater risk for respiratory mortality, while those in the APD-only group were additionally at greater risk for cardiovascular mortality. Biomarker analysis demonstrated a significant association of the APD-only group with CRP, and sRAGE demonstrated greatest significance with both the EPD-only and the combined APD-EPD groups. Interpretation: Among current and former smokers, individuals in the highest 2 deciles for mortality risk on the airway-predominant axis and the emphysema-predominant axis have unique associations to spirometric patterns, different imaging characteristics, biomarkers and causal mortality.

AB - Background: Previous attempts to explore the heterogeneity of chronic obstructive pulmonary disease (COPD) clustered individual patients using clinical, demographic, and disease features. We developed continuous multidimensional disease axes based on radiographic and spirometric variables that split into an airwaypredominant axis and an emphysema-predominant axis. Methods: The COPD Genetic Epidemiology study (COPDGene®) is a cohort of current and former smokers, > 45 years, with at least 10 pack years of smoking history. Spirometry measures, blood pressure and body mass were directly measured. Mortality was assessed through continuing longitudinal follow-up and cause of death was adjudicated. Among 8157 COPDGene® participants with complete spirometry and computed tomography (CT) measures, the top 2 deciles of the airway-predominant and emphysema-predominant axes previously identified were used to categorize individuals into 3 groups having the highest risk for mortality using Cox proportional hazard ratios. These groups were also assessed for causal mortality. Biomarkers of COPD (fibrinogen, soluble receptor for advanced glycation end products [sRAGE], C-reactive protein [CRP], clara cell secretory protein [CC16], surfactant-D [SP-D]) were compared by group. Findings: High-risk subtype classification was defined for 2638 COPDGene® participants who were in the highest 2 deciles of either the airway-predominant and/or emphysema-predominant axis (32% of the cohort). These high-risk participants fell into 3 groups: Airway-predominant disease only (APD-only), emphysemapredominant disease only (EPD-only) and combined APD-EPD. There was 26% mortality for the APD-only group, 21% mortality for the EPD-only group, and 54% mortality for the combined APD-EPD group. The APDonly group (n=1007) was younger, had a lower forced expiratory volume in 1 second (FEV1) percent (%) predicted and a strong association with the preserved ratio-impaired spirometry (PRISm) quadrant. The EPD-only group (n=1006) showed a relatively higher FEV1 % predicted and included largely GOLD stage 0, 1 and 2 partipants. Individuals in each of the 3 high-risk groups were at greater risk for respiratory mortality, while those in the APD-only group were additionally at greater risk for cardiovascular mortality. Biomarker analysis demonstrated a significant association of the APD-only group with CRP, and sRAGE demonstrated greatest significance with both the EPD-only and the combined APD-EPD groups. Interpretation: Among current and former smokers, individuals in the highest 2 deciles for mortality risk on the airway-predominant axis and the emphysema-predominant axis have unique associations to spirometric patterns, different imaging characteristics, biomarkers and causal mortality.

KW - Airwaypredominant disease

KW - Biomarkers

KW - COPD

KW - COPD Genetic Epidemiology

KW - COPDGene®

KW - Chronic obstructive pulmonary disease

KW - Emphysema-predominant disease

KW - Mortality

KW - PRISm

KW - Preserved ratio-impaired spirometry

KW - Subtypes

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AN - SCOPUS:85079799460

SN - 2372-952X

VL - 6

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EP - 413

JO - Chronic Obstructive Pulmonary Diseases

JF - Chronic Obstructive Pulmonary Diseases

IS - 5

ER -

Subtypes of COPD have unique distributions and differential risk of mortality

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