Human airway branch variation and chronic obstructive pulmonary disease

the MESA Lung and SPIROMICS investigators

doi:10.1073/pnas.1715564115

Human airway branch variation and chronic obstructive pulmonary disease

the MESA Lung and SPIROMICS investigators

School of Medicine

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

40 Scopus citations

Abstract

Susceptibility to chronic obstructive pulmonary disease (COPD) beyond cigarette smoking is incompletely understood, although several genetic variants associated with COPD are known to regulate airway branch development. We demonstrate that in vivo central airway branch variants are present in 26.5% of the general population, are unchanged over 10 y, and exhibit strong familial aggregation. The most common airway branch variant is associated with COPD in two cohorts (n = 5,054), with greater central airway bifurcation density, and with emphysema throughout the lung. The second most common airway branch variant is associated with COPD among smokers, with narrower airway lumens in all lobes, and with genetic polymorphisms within the FGF10 gene. We conclude that central airway branch variation, readily detected by computed tomography, is a biomarker of widely altered lung structure with a genetic basis and represents a COPD susceptibility factor.

Original language	English (US)
Pages (from-to)	E974-E981
Journal	Proceedings of the National Academy of Sciences of the United States of America
Volume	115
Issue number	5
DOIs	https://doi.org/10.1073/pnas.1715564115
State	Published - Jan 30 2018

Keywords

Airway branching
Chronic obstructive pulmonary disease
Computed tomography
Fibroblast growth factor

ASJC Scopus subject areas

General

Access to Document

10.1073/pnas.1715564115

Cite this

@article{029b349f2bd7493eace00afa47203a50,

title = "Human airway branch variation and chronic obstructive pulmonary disease",

abstract = "Susceptibility to chronic obstructive pulmonary disease (COPD) beyond cigarette smoking is incompletely understood, although several genetic variants associated with COPD are known to regulate airway branch development. We demonstrate that in vivo central airway branch variants are present in 26.5% of the general population, are unchanged over 10 y, and exhibit strong familial aggregation. The most common airway branch variant is associated with COPD in two cohorts (n = 5,054), with greater central airway bifurcation density, and with emphysema throughout the lung. The second most common airway branch variant is associated with COPD among smokers, with narrower airway lumens in all lobes, and with genetic polymorphisms within the FGF10 gene. We conclude that central airway branch variation, readily detected by computed tomography, is a biomarker of widely altered lung structure with a genetic basis and represents a COPD susceptibility factor.",

keywords = "Airway branching, Chronic obstructive pulmonary disease, Computed tomography, Fibroblast growth factor",

author = "{the MESA Lung and SPIROMICS investigators} and Smith, {Benjamin M.} and Hussein Traboulsi and Austin, {John H.M.} and Ani Manichaikul and Hoffman, {Eric A.} and Bleecker, {Eugene R.} and Cardoso, {Wellington V.} and Christopher Cooper and Couper, {David J.} and Dashnaw, {Stephen M.} and Jia Guo and Han, {Mei Lan K.} and Hansel, {Nadia N.} and Hughes, {Emlyn W.} and Jacobs, {David R.} and Kanner, {Richard E.} and Kaufman, {Joel D.} and Eric Kleerup and Lin, {Ching Long} and Kiang Liu and {Lo Cascio}, {Christian M.} and Martinez, {Fernando J.} and Nguyen, {Jennifer N.} and Prince, {Martin R.} and Stephen Rennard and Rich, {Stephen S.} and Leora Simon and Yanping Sun and Watson, {Karol E.} and Woodruff, {Prescott G.} and Baglole, {Carolyn J.} and Barr, {R. Graham}",

note = "Funding Information: We thank the other investigators, the staff, and the participants of the MESA Lung Study and SPIROMICS for their valuable contributions (a full list of participating MESA investigators and institutions can be found at https://www.mesa-nhlbi.org; more information about the study and how to access SPIROMICS data is available at www.spiromics.org) and acknowledge the following current and former investigators of the SPIROMICS sites and reading centers: Neil E. Alexis, PhD; Wayne H. Anderson, PhD; Richard C. Boucher, MD; Russell P. Bowler, MD, PhD; Elizabeth E. Carretta, MPH; Stephanie A. Christenson, MD; Alejandro P. Comellas, MD; Gerard J. Criner, MD; Ronald G. Crystal, MD; Jeffrey L. Curtis, MD; Claire M. Doerschuk, MD; Mark T. Dransfield, MD; Christine M. Freeman, PhD; Annette T. Hastie, PhD; Jerry A. Krishnan, MD, PhD; Lisa M. LaVange, PhD; Stephen C. Lazarus, MD; Deborah A. Meyers, PhD; John D. Newell, Jr, MD; Elizabeth C. Oelsner, MD, MPH; Wanda K. O{\textquoteright}Neal, PhD; Robert Paine, III, MD; Nirupama Putcha, MD, MHS; Donald P. Tashkin, MD; Mary Beth Scholand, MD; J. Michael Wells, MD; and Robert A. Wise, MD. The project officers from the Lung Division of the National Heart, Lung, and Blood Institute (NHLBI) were Lisa Postow, PhD, Thomas Croxton, PhD, MD, and Antonello Punturieri, MD, PhD. SPIROMICS was supported by NIH/NHLBI Contracts HHSN268200900013C, HHSN268200900014C, HHSN268200900015C, HHSN268200900016C, HHSN268200900017C, HHSN268200900018C HHSN268200900019C, and HHSN268200900020C, which were supplemented by contributions made through the Foundation for the NIH and COPD Foundation from AstraZeneca, Bellerophon Pharmaceuticals, Boehringer-Ingelheim Pharmaceuticals, Inc., Chiesi Farmaceutici SpA, Forest Research Institute, Inc., GlaxoSmithKline, Grifols Therapeutics, Inc., Ikaria, Inc., Nycomed GmbH, Takeda Pharmaceutical Company, Novartis Pharmaceuticals Corporation, Regeneron Pharmaceuticals, Inc., and Sanofi. Financial support was provided by NIH/NHLBI Grants R01-HL130506, R01-HL077612, R01-HL093081, R01-HL112986, RC1HL100543, RD831697, N01-HC-95159, N01-HC-95160, N01-HC-95169, N01-HC-95162, N01-HC-95164, U01-HL114494, N01-HC95159-HC95169, the NIH/NHLBI contracts named above, the McGill University Health Center Research Institute, and the Fonds de la recherche en sant{\'e} Qu{\'e}bec (Quebec Health Research Fund). Funding Information: ACKNOWLEDGMENTS. We thank the other investigators, the staff, and the participants of the MESA Lung Study and SPIROMICS for their valuable contributions (a full list of participating MESA investigators and institutions can be found at https://www.mesa-nhlbi.org; more information about the study and how to access SPIROMICS data is available at www.spiromics.org) and acknowledge the following current and former investigators of the SPIROMICS sites and reading centers: Neil E. Alexis, PhD; Wayne H. Anderson, PhD; Richard C. Boucher, MD; Russell P. Bowler, MD, PhD; Elizabeth E. Carretta, MPH; Stephanie A. Christenson, MD; Alejandro P. Comellas, MD; Gerard J. Criner, MD; Ronald G. Crystal, MD; Jeffrey L. Curtis, MD; Claire M. Doerschuk, MD; Mark T. Dransfield, MD; Christine M. Freeman, PhD; Annette T. Hastie, PhD; Jerry A. Krishnan, MD, PhD; Lisa M. LaVange, PhD; Stephen C. Lazarus, MD; Deborah A. Meyers, PhD; John D. Newell, Jr, MD; Elizabeth C. Oelsner, MD, MPH; Wanda K. O{\textquoteright}Neal, PhD; Robert Paine, III, MD; Nirupama Putcha, MD, MHS; Donald P. Tashkin, MD; Mary Beth Scholand, MD; J. Michael Wells, MD; and Robert A. Wise, MD. The project officers from the Lung Division of the National Heart, Lung, and Blood Institute (NHLBI) were Lisa Postow, PhD, Thomas Croxton, PhD, MD, and Antonello Punturieri, MD, PhD. SPIROMICS was supported by NIH/NHLBI Contracts HHSN268200900013C, HHSN268200900014C, HHSN268200900015C, HHSN268200900016C, HHSN268200900017C, HHSN268200900018C HHSN268200900019C, and HHSN268200900020C, which were supplemented by contributions made through the Foundation for the NIH and COPD Foundation from AstraZeneca, Bellerophon Pharmaceuticals, Boehringer-Ingelheim Pharmaceuticals, Inc., Chiesi Farmaceutici SpA, Forest Research Institute, Inc., GlaxoSmithKline, Grifols Therapeutics, Inc., Ikaria, Inc., Nycomed GmbH, Takeda Pharmaceutical Company, Novartis Pharmaceuticals Corporation, Regeneron Pharmaceuticals, Inc., and Sanofi. Financial support was provided by NIH/NHLBI Grants R01-HL130506, R01-HL077612, R01-HL093081, R01-HL112986, RC1HL100543, RD831697, N01-HC-95159, N01-HC-95160, N01-HC-95169, N01-HC-95162, N01-HC-95164, U01-HL114494, N01-HC95159-HC95169, the NIH/NHLBI contracts named above, the McGill University Health Center Research Institute, and the Fonds de la recherche en sant{\'e} Qu{\'e}bec (Quebec Health Research Fund).",

year = "2018",

month = jan,

day = "30",

doi = "10.1073/pnas.1715564115",

language = "English (US)",

volume = "115",

pages = "E974--E981",

journal = "Proceedings of the National Academy of Sciences of the United States of America",

issn = "0027-8424",

publisher = "National Academy of Sciences",

number = "5",

}

TY - JOUR

T1 - Human airway branch variation and chronic obstructive pulmonary disease

AU - the MESA Lung and SPIROMICS investigators

AU - Smith, Benjamin M.

AU - Traboulsi, Hussein

AU - Austin, John H.M.

AU - Manichaikul, Ani

AU - Hoffman, Eric A.

AU - Bleecker, Eugene R.

AU - Cardoso, Wellington V.

AU - Cooper, Christopher

AU - Couper, David J.

AU - Dashnaw, Stephen M.

AU - Guo, Jia

AU - Han, Mei Lan K.

AU - Hansel, Nadia N.

AU - Hughes, Emlyn W.

AU - Jacobs, David R.

AU - Kanner, Richard E.

AU - Kaufman, Joel D.

AU - Kleerup, Eric

AU - Lin, Ching Long

AU - Liu, Kiang

AU - Lo Cascio, Christian M.

AU - Martinez, Fernando J.

AU - Nguyen, Jennifer N.

AU - Prince, Martin R.

AU - Rennard, Stephen

AU - Rich, Stephen S.

AU - Simon, Leora

AU - Sun, Yanping

AU - Watson, Karol E.

AU - Woodruff, Prescott G.

AU - Baglole, Carolyn J.

AU - Barr, R. Graham

N1 - Funding Information: We thank the other investigators, the staff, and the participants of the MESA Lung Study and SPIROMICS for their valuable contributions (a full list of participating MESA investigators and institutions can be found at https://www.mesa-nhlbi.org; more information about the study and how to access SPIROMICS data is available at www.spiromics.org) and acknowledge the following current and former investigators of the SPIROMICS sites and reading centers: Neil E. Alexis, PhD; Wayne H. Anderson, PhD; Richard C. Boucher, MD; Russell P. Bowler, MD, PhD; Elizabeth E. Carretta, MPH; Stephanie A. Christenson, MD; Alejandro P. Comellas, MD; Gerard J. Criner, MD; Ronald G. Crystal, MD; Jeffrey L. Curtis, MD; Claire M. Doerschuk, MD; Mark T. Dransfield, MD; Christine M. Freeman, PhD; Annette T. Hastie, PhD; Jerry A. Krishnan, MD, PhD; Lisa M. LaVange, PhD; Stephen C. Lazarus, MD; Deborah A. Meyers, PhD; John D. Newell, Jr, MD; Elizabeth C. Oelsner, MD, MPH; Wanda K. O’Neal, PhD; Robert Paine, III, MD; Nirupama Putcha, MD, MHS; Donald P. Tashkin, MD; Mary Beth Scholand, MD; J. Michael Wells, MD; and Robert A. Wise, MD. The project officers from the Lung Division of the National Heart, Lung, and Blood Institute (NHLBI) were Lisa Postow, PhD, Thomas Croxton, PhD, MD, and Antonello Punturieri, MD, PhD. SPIROMICS was supported by NIH/NHLBI Contracts HHSN268200900013C, HHSN268200900014C, HHSN268200900015C, HHSN268200900016C, HHSN268200900017C, HHSN268200900018C HHSN268200900019C, and HHSN268200900020C, which were supplemented by contributions made through the Foundation for the NIH and COPD Foundation from AstraZeneca, Bellerophon Pharmaceuticals, Boehringer-Ingelheim Pharmaceuticals, Inc., Chiesi Farmaceutici SpA, Forest Research Institute, Inc., GlaxoSmithKline, Grifols Therapeutics, Inc., Ikaria, Inc., Nycomed GmbH, Takeda Pharmaceutical Company, Novartis Pharmaceuticals Corporation, Regeneron Pharmaceuticals, Inc., and Sanofi. Financial support was provided by NIH/NHLBI Grants R01-HL130506, R01-HL077612, R01-HL093081, R01-HL112986, RC1HL100543, RD831697, N01-HC-95159, N01-HC-95160, N01-HC-95169, N01-HC-95162, N01-HC-95164, U01-HL114494, N01-HC95159-HC95169, the NIH/NHLBI contracts named above, the McGill University Health Center Research Institute, and the Fonds de la recherche en santé Québec (Quebec Health Research Fund). Funding Information: ACKNOWLEDGMENTS. We thank the other investigators, the staff, and the participants of the MESA Lung Study and SPIROMICS for their valuable contributions (a full list of participating MESA investigators and institutions can be found at https://www.mesa-nhlbi.org; more information about the study and how to access SPIROMICS data is available at www.spiromics.org) and acknowledge the following current and former investigators of the SPIROMICS sites and reading centers: Neil E. Alexis, PhD; Wayne H. Anderson, PhD; Richard C. Boucher, MD; Russell P. Bowler, MD, PhD; Elizabeth E. Carretta, MPH; Stephanie A. Christenson, MD; Alejandro P. Comellas, MD; Gerard J. Criner, MD; Ronald G. Crystal, MD; Jeffrey L. Curtis, MD; Claire M. Doerschuk, MD; Mark T. Dransfield, MD; Christine M. Freeman, PhD; Annette T. Hastie, PhD; Jerry A. Krishnan, MD, PhD; Lisa M. LaVange, PhD; Stephen C. Lazarus, MD; Deborah A. Meyers, PhD; John D. Newell, Jr, MD; Elizabeth C. Oelsner, MD, MPH; Wanda K. O’Neal, PhD; Robert Paine, III, MD; Nirupama Putcha, MD, MHS; Donald P. Tashkin, MD; Mary Beth Scholand, MD; J. Michael Wells, MD; and Robert A. Wise, MD. The project officers from the Lung Division of the National Heart, Lung, and Blood Institute (NHLBI) were Lisa Postow, PhD, Thomas Croxton, PhD, MD, and Antonello Punturieri, MD, PhD. SPIROMICS was supported by NIH/NHLBI Contracts HHSN268200900013C, HHSN268200900014C, HHSN268200900015C, HHSN268200900016C, HHSN268200900017C, HHSN268200900018C HHSN268200900019C, and HHSN268200900020C, which were supplemented by contributions made through the Foundation for the NIH and COPD Foundation from AstraZeneca, Bellerophon Pharmaceuticals, Boehringer-Ingelheim Pharmaceuticals, Inc., Chiesi Farmaceutici SpA, Forest Research Institute, Inc., GlaxoSmithKline, Grifols Therapeutics, Inc., Ikaria, Inc., Nycomed GmbH, Takeda Pharmaceutical Company, Novartis Pharmaceuticals Corporation, Regeneron Pharmaceuticals, Inc., and Sanofi. Financial support was provided by NIH/NHLBI Grants R01-HL130506, R01-HL077612, R01-HL093081, R01-HL112986, RC1HL100543, RD831697, N01-HC-95159, N01-HC-95160, N01-HC-95169, N01-HC-95162, N01-HC-95164, U01-HL114494, N01-HC95159-HC95169, the NIH/NHLBI contracts named above, the McGill University Health Center Research Institute, and the Fonds de la recherche en santé Québec (Quebec Health Research Fund).

PY - 2018/1/30

Y1 - 2018/1/30

N2 - Susceptibility to chronic obstructive pulmonary disease (COPD) beyond cigarette smoking is incompletely understood, although several genetic variants associated with COPD are known to regulate airway branch development. We demonstrate that in vivo central airway branch variants are present in 26.5% of the general population, are unchanged over 10 y, and exhibit strong familial aggregation. The most common airway branch variant is associated with COPD in two cohorts (n = 5,054), with greater central airway bifurcation density, and with emphysema throughout the lung. The second most common airway branch variant is associated with COPD among smokers, with narrower airway lumens in all lobes, and with genetic polymorphisms within the FGF10 gene. We conclude that central airway branch variation, readily detected by computed tomography, is a biomarker of widely altered lung structure with a genetic basis and represents a COPD susceptibility factor.

AB - Susceptibility to chronic obstructive pulmonary disease (COPD) beyond cigarette smoking is incompletely understood, although several genetic variants associated with COPD are known to regulate airway branch development. We demonstrate that in vivo central airway branch variants are present in 26.5% of the general population, are unchanged over 10 y, and exhibit strong familial aggregation. The most common airway branch variant is associated with COPD in two cohorts (n = 5,054), with greater central airway bifurcation density, and with emphysema throughout the lung. The second most common airway branch variant is associated with COPD among smokers, with narrower airway lumens in all lobes, and with genetic polymorphisms within the FGF10 gene. We conclude that central airway branch variation, readily detected by computed tomography, is a biomarker of widely altered lung structure with a genetic basis and represents a COPD susceptibility factor.

KW - Airway branching

KW - Chronic obstructive pulmonary disease

KW - Computed tomography

KW - Fibroblast growth factor

UR - http://www.scopus.com/inward/record.url?scp=85041228991&partnerID=8YFLogxK

UR - http://www.scopus.com/inward/citedby.url?scp=85041228991&partnerID=8YFLogxK

U2 - 10.1073/pnas.1715564115

DO - 10.1073/pnas.1715564115

M3 - Article

C2 - 29339516

AN - SCOPUS:85041228991

SN - 0027-8424

VL - 115

SP - E974-E981

JO - Proceedings of the National Academy of Sciences of the United States of America

JF - Proceedings of the National Academy of Sciences of the United States of America

IS - 5

ER -

Human airway branch variation and chronic obstructive pulmonary disease

Abstract

Keywords

ASJC Scopus subject areas

Access to Document

Other files and links

Fingerprint

Cite this