A Meta-Analysis of Genome-Wide Association Scans Identifies IL18RAP, PTPN2, TAGAP, and PUS10 As Shared Risk Loci for Crohn's Disease and Celiac Disease

Crohn's disease (CD) and celiac disease (CelD) are chronic intestinal inflammatory diseases, involving genetic and environmental factors in their pathogenesis. The two diseases can co-occur within families, and studies suggest that CelD patients have a higher risk to develop CD than the general...

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Autores principales: Festen, Eleonora A. M., Goyette, Philippe, Green, Todd, Boucher, Gabrielle, Beauchamp, Claudine, Trynka, Gosia, Dubois, Patrick C., Lagacé, Caroline, Stokkers, Pieter C. F., Hommes, Daan W., Barisani, Donatella, Palmieri, Orazio, Annese, Vito, van Heel, David A., Weersma, Rinse K., Daly, Mark J., Wijmenga, Cisca, Rioux, John D.
Formato: Texto
Lenguaje:English
Publicado: Public Library of Science 2011
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3029251/
https://www.ncbi.nlm.nih.gov/pubmed/21298027
http://dx.doi.org/10.1371/journal.pgen.1001283
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author Festen, Eleonora A. M.
Goyette, Philippe
Green, Todd
Boucher, Gabrielle
Beauchamp, Claudine
Trynka, Gosia
Dubois, Patrick C.
Lagacé, Caroline
Stokkers, Pieter C. F.
Hommes, Daan W.
Barisani, Donatella
Palmieri, Orazio
Annese, Vito
van Heel, David A.
Weersma, Rinse K.
Daly, Mark J.
Wijmenga, Cisca
Rioux, John D.
author_facet Festen, Eleonora A. M.
Goyette, Philippe
Green, Todd
Boucher, Gabrielle
Beauchamp, Claudine
Trynka, Gosia
Dubois, Patrick C.
Lagacé, Caroline
Stokkers, Pieter C. F.
Hommes, Daan W.
Barisani, Donatella
Palmieri, Orazio
Annese, Vito
van Heel, David A.
Weersma, Rinse K.
Daly, Mark J.
Wijmenga, Cisca
Rioux, John D.
author_sort Festen, Eleonora A. M.
collection PubMed
description Crohn's disease (CD) and celiac disease (CelD) are chronic intestinal inflammatory diseases, involving genetic and environmental factors in their pathogenesis. The two diseases can co-occur within families, and studies suggest that CelD patients have a higher risk to develop CD than the general population. These observations suggest that CD and CelD may share common genetic risk loci. Two such shared loci, IL18RAP and PTPN2, have already been identified independently in these two diseases. The aim of our study was to explicitly identify shared risk loci for these diseases by combining results from genome-wide association study (GWAS) datasets of CD and CelD. Specifically, GWAS results from CelD (768 cases, 1,422 controls) and CD (3,230 cases, 4,829 controls) were combined in a meta-analysis. Nine independent regions had nominal association p-value <1.0×10(−5) in this meta-analysis and showed evidence of association to the individual diseases in the original scans (p-value <1×10(−2) in CelD and <1×10(−3 )in CD). These include the two previously reported shared loci, IL18RAP and PTPN2, with p-values of 3.37×10(−8) and 6.39×10(−9), respectively, in the meta-analysis. The other seven had not been reported as shared loci and thus were tested in additional CelD (3,149 cases and 4,714 controls) and CD (1,835 cases and 1,669 controls) cohorts. Two of these loci, TAGAP and PUS10, showed significant evidence of replication (Bonferroni corrected p-values <0.0071) in the combined CelD and CD replication cohorts and were firmly established as shared risk loci of genome-wide significance, with overall combined p-values of 1.55×10(−10) and 1.38×10(−11) respectively. Through a meta-analysis of GWAS data from CD and CelD, we have identified four shared risk loci: PTPN2, IL18RAP, TAGAP, and PUS10. The combined analysis of the two datasets provided the power, lacking in the individual GWAS for single diseases, to detect shared loci with a relatively small effect.
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spelling pubmed-30292512011-02-04 A Meta-Analysis of Genome-Wide Association Scans Identifies IL18RAP, PTPN2, TAGAP, and PUS10 As Shared Risk Loci for Crohn's Disease and Celiac Disease Festen, Eleonora A. M. Goyette, Philippe Green, Todd Boucher, Gabrielle Beauchamp, Claudine Trynka, Gosia Dubois, Patrick C. Lagacé, Caroline Stokkers, Pieter C. F. Hommes, Daan W. Barisani, Donatella Palmieri, Orazio Annese, Vito van Heel, David A. Weersma, Rinse K. Daly, Mark J. Wijmenga, Cisca Rioux, John D. PLoS Genet Research Article Crohn's disease (CD) and celiac disease (CelD) are chronic intestinal inflammatory diseases, involving genetic and environmental factors in their pathogenesis. The two diseases can co-occur within families, and studies suggest that CelD patients have a higher risk to develop CD than the general population. These observations suggest that CD and CelD may share common genetic risk loci. Two such shared loci, IL18RAP and PTPN2, have already been identified independently in these two diseases. The aim of our study was to explicitly identify shared risk loci for these diseases by combining results from genome-wide association study (GWAS) datasets of CD and CelD. Specifically, GWAS results from CelD (768 cases, 1,422 controls) and CD (3,230 cases, 4,829 controls) were combined in a meta-analysis. Nine independent regions had nominal association p-value <1.0×10(−5) in this meta-analysis and showed evidence of association to the individual diseases in the original scans (p-value <1×10(−2) in CelD and <1×10(−3 )in CD). These include the two previously reported shared loci, IL18RAP and PTPN2, with p-values of 3.37×10(−8) and 6.39×10(−9), respectively, in the meta-analysis. The other seven had not been reported as shared loci and thus were tested in additional CelD (3,149 cases and 4,714 controls) and CD (1,835 cases and 1,669 controls) cohorts. Two of these loci, TAGAP and PUS10, showed significant evidence of replication (Bonferroni corrected p-values <0.0071) in the combined CelD and CD replication cohorts and were firmly established as shared risk loci of genome-wide significance, with overall combined p-values of 1.55×10(−10) and 1.38×10(−11) respectively. Through a meta-analysis of GWAS data from CD and CelD, we have identified four shared risk loci: PTPN2, IL18RAP, TAGAP, and PUS10. The combined analysis of the two datasets provided the power, lacking in the individual GWAS for single diseases, to detect shared loci with a relatively small effect. Public Library of Science 2011-01-27 /pmc/articles/PMC3029251/ /pubmed/21298027 http://dx.doi.org/10.1371/journal.pgen.1001283 Text en Festen et al. This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Festen, Eleonora A. M.
Goyette, Philippe
Green, Todd
Boucher, Gabrielle
Beauchamp, Claudine
Trynka, Gosia
Dubois, Patrick C.
Lagacé, Caroline
Stokkers, Pieter C. F.
Hommes, Daan W.
Barisani, Donatella
Palmieri, Orazio
Annese, Vito
van Heel, David A.
Weersma, Rinse K.
Daly, Mark J.
Wijmenga, Cisca
Rioux, John D.
A Meta-Analysis of Genome-Wide Association Scans Identifies IL18RAP, PTPN2, TAGAP, and PUS10 As Shared Risk Loci for Crohn's Disease and Celiac Disease
title A Meta-Analysis of Genome-Wide Association Scans Identifies IL18RAP, PTPN2, TAGAP, and PUS10 As Shared Risk Loci for Crohn's Disease and Celiac Disease
title_full A Meta-Analysis of Genome-Wide Association Scans Identifies IL18RAP, PTPN2, TAGAP, and PUS10 As Shared Risk Loci for Crohn's Disease and Celiac Disease
title_fullStr A Meta-Analysis of Genome-Wide Association Scans Identifies IL18RAP, PTPN2, TAGAP, and PUS10 As Shared Risk Loci for Crohn's Disease and Celiac Disease
title_full_unstemmed A Meta-Analysis of Genome-Wide Association Scans Identifies IL18RAP, PTPN2, TAGAP, and PUS10 As Shared Risk Loci for Crohn's Disease and Celiac Disease
title_short A Meta-Analysis of Genome-Wide Association Scans Identifies IL18RAP, PTPN2, TAGAP, and PUS10 As Shared Risk Loci for Crohn's Disease and Celiac Disease
title_sort meta-analysis of genome-wide association scans identifies il18rap, ptpn2, tagap, and pus10 as shared risk loci for crohn's disease and celiac disease
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3029251/
https://www.ncbi.nlm.nih.gov/pubmed/21298027
http://dx.doi.org/10.1371/journal.pgen.1001283
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