Multicentric Genome-Wide Association Study for Primary Spontaneous Pneumothorax.
Despite elevated incidence and recurrence rates for Primary Spontaneous Pneumothorax (PSP), little is known about its etiology, and the genetics of idiopathic PSP remains unexplored. To identify genetic variants contributing to sporadic PSP risk, we conducted the first PSP genome-wide association st...
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doaj-e147678741ff48b6a12d26fadcef9d3f2020-11-24T21:35:15ZengPublic Library of Science (PLoS)PLoS ONE1932-62032016-01-01115e015610310.1371/journal.pone.0156103Multicentric Genome-Wide Association Study for Primary Spontaneous Pneumothorax.Inês SousaPatrícia AbrantesVânia FranciscoGilberto TeixeiraMarta MonteiroJoão NevesAna NorteCarlos Robalo CordeiroJoão Moura E SáErnestina ReisPatrícia SantosManuela OliveiraSusana SousaMarta FradinhoFilipa MalheiroLuís NegrãoSalvato FeijóSofia A OliveiraDespite elevated incidence and recurrence rates for Primary Spontaneous Pneumothorax (PSP), little is known about its etiology, and the genetics of idiopathic PSP remains unexplored. To identify genetic variants contributing to sporadic PSP risk, we conducted the first PSP genome-wide association study. Two replicate pools of 92 Portuguese PSP cases and of 129 age- and sex-matched controls were allelotyped in triplicate on the Affymetrix Human SNP Array 6.0 arrays. Markers passing quality control were ranked by relative allele score difference between cases and controls (|RASdiff|), by a novel cluster method and by a combined Z-test. 101 single nucleotide polymorphisms (SNPs) were selected using these three approaches for technical validation by individual genotyping in the discovery dataset. 87 out of 94 successfully tested SNPs were nominally associated in the discovery dataset. Replication of the 87 technically validated SNPs was then carried out in an independent replication dataset of 100 Portuguese cases and 425 controls. The intergenic rs4733649 SNP in chromosome 8 (between LINC00824 and LINC00977) was associated with PSP in the discovery (P = 4.07E-03, ORC[95% CI] = 1.88[1.22-2.89]), replication (P = 1.50E-02, ORC[95% CI] = 1.50[1.08-2.09]) and combined datasets (P = 8.61E-05, ORC[95% CI] = 1.65[1.29-2.13]). This study identified for the first time one genetic risk factor for sporadic PSP, but future studies are warranted to further confirm this finding in other populations and uncover its functional role in PSP pathogenesis.http://europepmc.org/articles/PMC4874577?pdf=render |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Inês Sousa Patrícia Abrantes Vânia Francisco Gilberto Teixeira Marta Monteiro João Neves Ana Norte Carlos Robalo Cordeiro João Moura E Sá Ernestina Reis Patrícia Santos Manuela Oliveira Susana Sousa Marta Fradinho Filipa Malheiro Luís Negrão Salvato Feijó Sofia A Oliveira |
spellingShingle |
Inês Sousa Patrícia Abrantes Vânia Francisco Gilberto Teixeira Marta Monteiro João Neves Ana Norte Carlos Robalo Cordeiro João Moura E Sá Ernestina Reis Patrícia Santos Manuela Oliveira Susana Sousa Marta Fradinho Filipa Malheiro Luís Negrão Salvato Feijó Sofia A Oliveira Multicentric Genome-Wide Association Study for Primary Spontaneous Pneumothorax. PLoS ONE |
author_facet |
Inês Sousa Patrícia Abrantes Vânia Francisco Gilberto Teixeira Marta Monteiro João Neves Ana Norte Carlos Robalo Cordeiro João Moura E Sá Ernestina Reis Patrícia Santos Manuela Oliveira Susana Sousa Marta Fradinho Filipa Malheiro Luís Negrão Salvato Feijó Sofia A Oliveira |
author_sort |
Inês Sousa |
title |
Multicentric Genome-Wide Association Study for Primary Spontaneous Pneumothorax. |
title_short |
Multicentric Genome-Wide Association Study for Primary Spontaneous Pneumothorax. |
title_full |
Multicentric Genome-Wide Association Study for Primary Spontaneous Pneumothorax. |
title_fullStr |
Multicentric Genome-Wide Association Study for Primary Spontaneous Pneumothorax. |
title_full_unstemmed |
Multicentric Genome-Wide Association Study for Primary Spontaneous Pneumothorax. |
title_sort |
multicentric genome-wide association study for primary spontaneous pneumothorax. |
publisher |
Public Library of Science (PLoS) |
series |
PLoS ONE |
issn |
1932-6203 |
publishDate |
2016-01-01 |
description |
Despite elevated incidence and recurrence rates for Primary Spontaneous Pneumothorax (PSP), little is known about its etiology, and the genetics of idiopathic PSP remains unexplored. To identify genetic variants contributing to sporadic PSP risk, we conducted the first PSP genome-wide association study. Two replicate pools of 92 Portuguese PSP cases and of 129 age- and sex-matched controls were allelotyped in triplicate on the Affymetrix Human SNP Array 6.0 arrays. Markers passing quality control were ranked by relative allele score difference between cases and controls (|RASdiff|), by a novel cluster method and by a combined Z-test. 101 single nucleotide polymorphisms (SNPs) were selected using these three approaches for technical validation by individual genotyping in the discovery dataset. 87 out of 94 successfully tested SNPs were nominally associated in the discovery dataset. Replication of the 87 technically validated SNPs was then carried out in an independent replication dataset of 100 Portuguese cases and 425 controls. The intergenic rs4733649 SNP in chromosome 8 (between LINC00824 and LINC00977) was associated with PSP in the discovery (P = 4.07E-03, ORC[95% CI] = 1.88[1.22-2.89]), replication (P = 1.50E-02, ORC[95% CI] = 1.50[1.08-2.09]) and combined datasets (P = 8.61E-05, ORC[95% CI] = 1.65[1.29-2.13]). This study identified for the first time one genetic risk factor for sporadic PSP, but future studies are warranted to further confirm this finding in other populations and uncover its functional role in PSP pathogenesis. |
url |
http://europepmc.org/articles/PMC4874577?pdf=render |
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