Whole Exome Re-Sequencing Implicates CCDC38 and Cilia Structure and Function in Resistance to Smoking Related Airflow Obstruction

Wain, Louise V.; Sayers, Ian; Soler Artigas, Mar�a; Portelli, Michael A.; Zeggini, Eleftheria; Obeidat, Ma�en; Sin, Don D.; Boss�, Yohan; Nickle, David C.; Brandsma, Corry-Anke; Malarstig, Anders; Vangjeli, Ciara; Jelingsky, Scott A.; John, Sally; Kilty, Iain; McKeever, Tricia M.; Shrine, Nick; Cook, James P.; Patel, Shrina; Spector, Tim D.; Hollox, Edward J.; Hall, Ian P.; Tobin, Martin D.

doi:10.1371/journal.pgen.1004314

Whole Exome Re-Sequencing Implicates CCDC38 and Cilia Structure and Function in Resistance to Smoking Related Airflow Obstruction

Wain, Louise V.; Sayers, Ian; Soler Artigas, Mar�a; Portelli, Michael A.; Zeggini, Eleftheria; Obeidat, Ma�en; Sin, Don D.; Boss�, Yohan; Nickle, David C.; Brandsma, Corry-Anke; Malarstig, Anders; Vangjeli, Ciara; Jelingsky, Scott A.; John, Sally; Kilty, Iain; McKeever, Tricia M.; Shrine, Nick; Cook, James P.; Patel, Shrina; Spector, Tim D.; Hollox, Edward J.; Hall, Ian P.; Tobin, Martin D.

Authors

Louise V. Wain

Professor IAN SAYERS ian.sayers@nottingham.ac.uk
Professor of Respiratory Molecular Genetics

Mar�a Soler Artigas

Michael A. Portelli

Eleftheria Zeggini

Ma�en Obeidat

Don D. Sin

Yohan Boss�

David C. Nickle

Corry-Anke Brandsma

Anders Malarstig

Ciara Vangjeli

Scott A. Jelingsky

Sally John

Iain Kilty

TRICIA MCKEEVER tricia.mckeever@nottingham.ac.uk
Professor of Epidemiology and Medical Statistics

Nick Shrine

James P. Cook

Shrina Patel

Tim D. Spector

Edward J. Hollox

IAN HALL IAN.HALL@NOTTINGHAM.AC.UK
Professor of Molecular Medicine

Martin D. Tobin

Contributors

Greg Gibson
Editor

Abstract

Chronic obstructive pulmonary disease (COPD) is a leading cause of global morbidity and mortality and, whilst smoking remains the single most important risk factor, COPD risk is heritable. Of 26 independent genomic regions showing association with lung function in genome-wide association studies, eleven have been reported to show association with airflow obstruction. Although the main risk factor for COPD is smoking, some individuals are observed to have a high forced expired volume in 1 second (FEV1) despite many years of heavy smoking. We # hypothesised that these ‘‘resistant smokers’’ may harbour variants which protect against lung function decline caused by smoking and provide insight into the genetic determinants of lung health. We undertook whole exome re sequencing of 100 heavy smokers who had healthy lung function given their age, sex, height and smoking history and applied three complementary approaches to explore the genetic architecture of smoking resistance. Firstly, we identified novel functional variants in the ‘‘resistant smokers’’ and looked for enrichment of these novel variants within biological pathways. Secondly, we undertook association testing of all exonic variants individually with two independent control sets. Thirdly, we undertook gene-based association testing of all exonic variants. Our strongest signal of association with smoking resistance for a non-synonymous SNP was for rs10859974 (P = 2.3461024) in CCDC38, a gene which has previously been reported to show association with FEV1/FVC, and we demonstrate moderate expression of CCDC38 in bronchial epithelial cells. We identified an enrichment of novel putatively functional variants in genes related to cilia structure and function in resistant smokers. Ciliary function abnormalities are known to be associated with both smoking and reduced mucociliary clearance in patients with COPD. We suggest that genetic influences on the development or function of cilia in the bronchial epithelium may affect growth of cilia or the extent of damage caused by tobacco smoke.

Citation

Wain, L. V., Sayers, I., Soler Artigas, M., Portelli, M. A., Zeggini, E., Obeidat, M., …Tobin, M. D. (2014). Whole Exome Re-Sequencing Implicates CCDC38 and Cilia Structure and Function in Resistance to Smoking Related Airflow Obstruction. PLoS Genetics, 10(5), Article e1004314. https://doi.org/10.1371/journal.pgen.1004314

Journal Article Type	Article
Acceptance Date	Mar 6, 2014
Online Publication Date	May 1, 2014
Publication Date	May 1, 2014
Deposit Date	Apr 6, 2016
Publicly Available Date	Apr 6, 2016
Journal	PLoS Genetics
Print ISSN	1553-7390
Electronic ISSN	1553-7404
Publisher	Public Library of Science
Peer Reviewed	Peer Reviewed
Volume	10
Issue	5
Article Number	e1004314
DOI	https://doi.org/10.1371/journal.pgen.1004314
Public URL	https://nottingham-repository.worktribe.com/output/726269
Publisher URL	http://journals.plos.org/plosgenetics/article?id=10.1371/journal.pgen.1004314
Contract Date	Apr 6, 2016