Genetic association and transcriptome integration identify contributing genes and tissues at cystic fibrosis modifier loci

Cystic Fibrosis (CF) exhibits morbidity in several organs, including progressive lung disease in all patients and intestinal obstruction at birth (meconium ileus) in ~15%. Individuals with the same causal CFTR mutations show variable disease presentation which is partly attributed to modifier genes....

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Autores principales: Gong, Jiafen, Wang, Fan, Xiao, Bowei, Panjwani, Naim, Lin, Fan, Keenan, Katherine, Avolio, Julie, Esmaeili, Mohsen, Zhang, Lin, He, Gengming, Soave, David, Mastromatteo, Scott, Baskurt, Zeynep, Kim, Sangook, O’Neal, Wanda K., Polineni, Deepika, Blackman, Scott M., Corvol, Harriet, Cutting, Garry R., Drumm, Mitchell, Knowles, Michael R., Rommens, Johanna M., Sun, Lei, Strug, Lisa J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2019
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6407791/
https://www.ncbi.nlm.nih.gov/pubmed/30807572
http://dx.doi.org/10.1371/journal.pgen.1008007
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author Gong, Jiafen
Wang, Fan
Xiao, Bowei
Panjwani, Naim
Lin, Fan
Keenan, Katherine
Avolio, Julie
Esmaeili, Mohsen
Zhang, Lin
He, Gengming
Soave, David
Mastromatteo, Scott
Baskurt, Zeynep
Kim, Sangook
O’Neal, Wanda K.
Polineni, Deepika
Blackman, Scott M.
Corvol, Harriet
Cutting, Garry R.
Drumm, Mitchell
Knowles, Michael R.
Rommens, Johanna M.
Sun, Lei
Strug, Lisa J.
author_facet Gong, Jiafen
Wang, Fan
Xiao, Bowei
Panjwani, Naim
Lin, Fan
Keenan, Katherine
Avolio, Julie
Esmaeili, Mohsen
Zhang, Lin
He, Gengming
Soave, David
Mastromatteo, Scott
Baskurt, Zeynep
Kim, Sangook
O’Neal, Wanda K.
Polineni, Deepika
Blackman, Scott M.
Corvol, Harriet
Cutting, Garry R.
Drumm, Mitchell
Knowles, Michael R.
Rommens, Johanna M.
Sun, Lei
Strug, Lisa J.
author_sort Gong, Jiafen
collection PubMed
description Cystic Fibrosis (CF) exhibits morbidity in several organs, including progressive lung disease in all patients and intestinal obstruction at birth (meconium ileus) in ~15%. Individuals with the same causal CFTR mutations show variable disease presentation which is partly attributed to modifier genes. With >6,500 participants from the International CF Gene Modifier Consortium, genome-wide association investigation identified a new modifier locus for meconium ileus encompassing ATP12A on chromosome 13 (min p = 3.83x10(-10)); replicated loci encompassing SLC6A14 on chromosome X and SLC26A9 on chromosome 1, (min p<2.2x10(-16), 2.81x10(−11), respectively); and replicated a suggestive locus on chromosome 7 near PRSS1 (min p = 2.55x10(-7)). PRSS1 is exclusively expressed in the exocrine pancreas and was previously associated with non-CF pancreatitis with functional characterization demonstrating impact on PRSS1 gene expression. We thus asked whether the other meconium ileus modifier loci impact gene expression and in which organ. We developed and applied a colocalization framework called the Simple Sum (SS) that integrates regulatory and genetic association information, and also contrasts colocalization evidence across tissues or genes. The associated modifier loci colocalized with expression quantitative trait loci (eQTLs) for ATP12A (p = 3.35x10(-8)), SLC6A14 (p = 1.12x10(-10)) and SLC26A9 (p = 4.48x10(-5)) in the pancreas, even though meconium ileus manifests in the intestine. The meconium ileus susceptibility locus on chromosome X appeared shifted in location from a previously identified locus for CF lung disease severity. Using the SS we integrated the lung disease association locus with eQTLs from nasal epithelia of 63 CF participants and demonstrated evidence of colocalization with airway-specific regulation of SLC6A14 (p = 2.3x10(-4)). Cystic Fibrosis is realizing the promise of personalized medicine, and identification of the contributing organ and understanding of tissue specificity for a gene modifier is essential for the next phase of personalizing therapeutic strategies.
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spelling pubmed-64077912019-03-17 Genetic association and transcriptome integration identify contributing genes and tissues at cystic fibrosis modifier loci Gong, Jiafen Wang, Fan Xiao, Bowei Panjwani, Naim Lin, Fan Keenan, Katherine Avolio, Julie Esmaeili, Mohsen Zhang, Lin He, Gengming Soave, David Mastromatteo, Scott Baskurt, Zeynep Kim, Sangook O’Neal, Wanda K. Polineni, Deepika Blackman, Scott M. Corvol, Harriet Cutting, Garry R. Drumm, Mitchell Knowles, Michael R. Rommens, Johanna M. Sun, Lei Strug, Lisa J. PLoS Genet Research Article Cystic Fibrosis (CF) exhibits morbidity in several organs, including progressive lung disease in all patients and intestinal obstruction at birth (meconium ileus) in ~15%. Individuals with the same causal CFTR mutations show variable disease presentation which is partly attributed to modifier genes. With >6,500 participants from the International CF Gene Modifier Consortium, genome-wide association investigation identified a new modifier locus for meconium ileus encompassing ATP12A on chromosome 13 (min p = 3.83x10(-10)); replicated loci encompassing SLC6A14 on chromosome X and SLC26A9 on chromosome 1, (min p<2.2x10(-16), 2.81x10(−11), respectively); and replicated a suggestive locus on chromosome 7 near PRSS1 (min p = 2.55x10(-7)). PRSS1 is exclusively expressed in the exocrine pancreas and was previously associated with non-CF pancreatitis with functional characterization demonstrating impact on PRSS1 gene expression. We thus asked whether the other meconium ileus modifier loci impact gene expression and in which organ. We developed and applied a colocalization framework called the Simple Sum (SS) that integrates regulatory and genetic association information, and also contrasts colocalization evidence across tissues or genes. The associated modifier loci colocalized with expression quantitative trait loci (eQTLs) for ATP12A (p = 3.35x10(-8)), SLC6A14 (p = 1.12x10(-10)) and SLC26A9 (p = 4.48x10(-5)) in the pancreas, even though meconium ileus manifests in the intestine. The meconium ileus susceptibility locus on chromosome X appeared shifted in location from a previously identified locus for CF lung disease severity. Using the SS we integrated the lung disease association locus with eQTLs from nasal epithelia of 63 CF participants and demonstrated evidence of colocalization with airway-specific regulation of SLC6A14 (p = 2.3x10(-4)). Cystic Fibrosis is realizing the promise of personalized medicine, and identification of the contributing organ and understanding of tissue specificity for a gene modifier is essential for the next phase of personalizing therapeutic strategies. Public Library of Science 2019-02-26 /pmc/articles/PMC6407791/ /pubmed/30807572 http://dx.doi.org/10.1371/journal.pgen.1008007 Text en © 2019 Gong et al http://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Gong, Jiafen
Wang, Fan
Xiao, Bowei
Panjwani, Naim
Lin, Fan
Keenan, Katherine
Avolio, Julie
Esmaeili, Mohsen
Zhang, Lin
He, Gengming
Soave, David
Mastromatteo, Scott
Baskurt, Zeynep
Kim, Sangook
O’Neal, Wanda K.
Polineni, Deepika
Blackman, Scott M.
Corvol, Harriet
Cutting, Garry R.
Drumm, Mitchell
Knowles, Michael R.
Rommens, Johanna M.
Sun, Lei
Strug, Lisa J.
Genetic association and transcriptome integration identify contributing genes and tissues at cystic fibrosis modifier loci
title Genetic association and transcriptome integration identify contributing genes and tissues at cystic fibrosis modifier loci
title_full Genetic association and transcriptome integration identify contributing genes and tissues at cystic fibrosis modifier loci
title_fullStr Genetic association and transcriptome integration identify contributing genes and tissues at cystic fibrosis modifier loci
title_full_unstemmed Genetic association and transcriptome integration identify contributing genes and tissues at cystic fibrosis modifier loci
title_short Genetic association and transcriptome integration identify contributing genes and tissues at cystic fibrosis modifier loci
title_sort genetic association and transcriptome integration identify contributing genes and tissues at cystic fibrosis modifier loci
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6407791/
https://www.ncbi.nlm.nih.gov/pubmed/30807572
http://dx.doi.org/10.1371/journal.pgen.1008007
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