IL23R variation determines susceptibility but not disease phenotype in inflammatory bowel disease

M Tremelling; F Cummings; S A Fisher; J Mansfield; R Gwilliam; A Keniry; E R Nimmo; H Drummond; C M Onnie; N J Prescott; J Sanderson; F Bredin; C Berzuini; A Forbes; C M Lewis; L Cardon; P Deloukas; D Jewell; C G Mathew; M Parkes; J Satsangi

doi:10.1053/j.gastro.2007.02.051

IL23R variation determines susceptibility but not disease phenotype in inflammatory bowel disease

M Tremelling, F Cummings, S A Fisher, J Mansfield, R Gwilliam, A Keniry, E R Nimmo, H Drummond, C M Onnie, N J Prescott, J Sanderson, F Bredin, C Berzuini, A Forbes, C M Lewis, L Cardon, P Deloukas, D Jewell, C G Mathew, M ParkesJ Satsangi

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Abstract

Background & Aims: Identification of inflammatory bowel disease (IBD) susceptibility genes is key to understanding pathogenic mechanisms. Recently, the North American IBD Genetics Consortium provided compelling evidence for an association between ileal Crohn's disease (CD) and the IL23R gene using genome-wide association scanning. External replication is a priority, both to confirm this finding in other populations and to validate this new technique. We tested for association between IL23R and IBD in a large independent UK panel to determine the size of the effect and explore subphenotype correlation and interaction with CARD15. Methods: Eight single nucleotide polymorphism markers in IL23R tested in the North American study were genotyped in 1902 cases of Crohn's disease (CD), 975 cases of ulcerative colitis (UC), and 1345 controls using MassARRAY. Data were analyzed using X-2 statistics, and subgroup association was sought. Results: A highly significant association with CD was observed, with the strongest signal at coding variant Arg381Gln (allele frequency, 2.5% in CD vs 6.2% in controls [P = 1.1 X 10(-1)2]; odds ratio, 0.38; 95% confidence interval, 0.29 - 0.50). A weaker effect was seen in UC (allele frequency, 4.6%; odds ratio, 0.73; 95% confidence interval, 0.55-0.96). Analysis accounting for Arg381Gln suggested that other loci within IL23R also influence IBD susceptibility. Within CD, there were no subphenotype associations or evidence of interaction with CARD15. Conclusions: This study shows an association between IL23R and all sub-phenotypes of CD with a smaller effect on UC. This extends the findings of the North American study, providing clear evidence that genome-wide association scanning can successfully identify true complex disease genes

Original language	English
Pages (from-to)	1657 - 1664
Number of pages	8
Journal	Gastroenterology
Volume	132
Issue number	5
DOIs	https://doi.org/10.1053/j.gastro.2007.02.051
Publication status	Published - May 2007

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Tremelling, M., Cummings, F., Fisher, S. A., Mansfield, J., Gwilliam, R., Keniry, A., Nimmo, E. R., Drummond, H., Onnie, C. M., Prescott, N. J., Sanderson, J., Bredin, F., Berzuini, C., Forbes, A., Lewis, C. M., Cardon, L., Deloukas, P., Jewell, D., Mathew, C. G., ... Satsangi, J. (2007). IL23R variation determines susceptibility but not disease phenotype in inflammatory bowel disease. Gastroenterology, 132(5), 1657 - 1664. https://doi.org/10.1053/j.gastro.2007.02.051

@article{c37b05b119e846de8b67a0787adccf98,

title = "IL23R variation determines susceptibility but not disease phenotype in inflammatory bowel disease",

abstract = "Background & Aims: Identification of inflammatory bowel disease (IBD) susceptibility genes is key to understanding pathogenic mechanisms. Recently, the North American IBD Genetics Consortium provided compelling evidence for an association between ileal Crohn's disease (CD) and the IL23R gene using genome-wide association scanning. External replication is a priority, both to confirm this finding in other populations and to validate this new technique. We tested for association between IL23R and IBD in a large independent UK panel to determine the size of the effect and explore subphenotype correlation and interaction with CARD15. Methods: Eight single nucleotide polymorphism markers in IL23R tested in the North American study were genotyped in 1902 cases of Crohn's disease (CD), 975 cases of ulcerative colitis (UC), and 1345 controls using MassARRAY. Data were analyzed using X-2 statistics, and subgroup association was sought. Results: A highly significant association with CD was observed, with the strongest signal at coding variant Arg381Gln (allele frequency, 2.5% in CD vs 6.2% in controls [P = 1.1 X 10(-1)2]; odds ratio, 0.38; 95% confidence interval, 0.29 - 0.50). A weaker effect was seen in UC (allele frequency, 4.6%; odds ratio, 0.73; 95% confidence interval, 0.55-0.96). Analysis accounting for Arg381Gln suggested that other loci within IL23R also influence IBD susceptibility. Within CD, there were no subphenotype associations or evidence of interaction with CARD15. Conclusions: This study shows an association between IL23R and all sub-phenotypes of CD with a smaller effect on UC. This extends the findings of the North American study, providing clear evidence that genome-wide association scanning can successfully identify true complex disease genes",

author = "M Tremelling and F Cummings and Fisher, {S A} and J Mansfield and R Gwilliam and A Keniry and Nimmo, {E R} and H Drummond and Onnie, {C M} and Prescott, {N J} and J Sanderson and F Bredin and C Berzuini and A Forbes and Lewis, {C M} and L Cardon and P Deloukas and D Jewell and Mathew, {C G} and M Parkes and J Satsangi",

year = "2007",

month = may,

doi = "10.1053/j.gastro.2007.02.051",

language = "English",

volume = "132",

pages = "1657 -- 1664",

journal = "Gastroenterology",

issn = "1528-0012",

publisher = "WB Saunders",

number = "5",

}

Tremelling, M, Cummings, F, Fisher, SA, Mansfield, J, Gwilliam, R, Keniry, A, Nimmo, ER, Drummond, H, Onnie, CM , Prescott, NJ , Sanderson, J, Bredin, F, Berzuini, C, Forbes, A, Lewis, CM, Cardon, L, Deloukas, P, Jewell, D, Mathew, CG, Parkes, M & Satsangi, J 2007, 'IL23R variation determines susceptibility but not disease phenotype in inflammatory bowel disease', Gastroenterology, vol. 132, no. 5, pp. 1657 - 1664. https://doi.org/10.1053/j.gastro.2007.02.051

TY - JOUR

T1 - IL23R variation determines susceptibility but not disease phenotype in inflammatory bowel disease

AU - Tremelling, M

AU - Cummings, F

AU - Fisher, S A

AU - Mansfield, J

AU - Gwilliam, R

AU - Keniry, A

AU - Nimmo, E R

AU - Drummond, H

AU - Onnie, C M

AU - Prescott, N J

AU - Sanderson, J

AU - Bredin, F

AU - Berzuini, C

AU - Forbes, A

AU - Lewis, C M

AU - Cardon, L

AU - Deloukas, P

AU - Jewell, D

AU - Mathew, C G

AU - Parkes, M

AU - Satsangi, J

PY - 2007/5

Y1 - 2007/5

N2 - Background & Aims: Identification of inflammatory bowel disease (IBD) susceptibility genes is key to understanding pathogenic mechanisms. Recently, the North American IBD Genetics Consortium provided compelling evidence for an association between ileal Crohn's disease (CD) and the IL23R gene using genome-wide association scanning. External replication is a priority, both to confirm this finding in other populations and to validate this new technique. We tested for association between IL23R and IBD in a large independent UK panel to determine the size of the effect and explore subphenotype correlation and interaction with CARD15. Methods: Eight single nucleotide polymorphism markers in IL23R tested in the North American study were genotyped in 1902 cases of Crohn's disease (CD), 975 cases of ulcerative colitis (UC), and 1345 controls using MassARRAY. Data were analyzed using X-2 statistics, and subgroup association was sought. Results: A highly significant association with CD was observed, with the strongest signal at coding variant Arg381Gln (allele frequency, 2.5% in CD vs 6.2% in controls [P = 1.1 X 10(-1)2]; odds ratio, 0.38; 95% confidence interval, 0.29 - 0.50). A weaker effect was seen in UC (allele frequency, 4.6%; odds ratio, 0.73; 95% confidence interval, 0.55-0.96). Analysis accounting for Arg381Gln suggested that other loci within IL23R also influence IBD susceptibility. Within CD, there were no subphenotype associations or evidence of interaction with CARD15. Conclusions: This study shows an association between IL23R and all sub-phenotypes of CD with a smaller effect on UC. This extends the findings of the North American study, providing clear evidence that genome-wide association scanning can successfully identify true complex disease genes

AB - Background & Aims: Identification of inflammatory bowel disease (IBD) susceptibility genes is key to understanding pathogenic mechanisms. Recently, the North American IBD Genetics Consortium provided compelling evidence for an association between ileal Crohn's disease (CD) and the IL23R gene using genome-wide association scanning. External replication is a priority, both to confirm this finding in other populations and to validate this new technique. We tested for association between IL23R and IBD in a large independent UK panel to determine the size of the effect and explore subphenotype correlation and interaction with CARD15. Methods: Eight single nucleotide polymorphism markers in IL23R tested in the North American study were genotyped in 1902 cases of Crohn's disease (CD), 975 cases of ulcerative colitis (UC), and 1345 controls using MassARRAY. Data were analyzed using X-2 statistics, and subgroup association was sought. Results: A highly significant association with CD was observed, with the strongest signal at coding variant Arg381Gln (allele frequency, 2.5% in CD vs 6.2% in controls [P = 1.1 X 10(-1)2]; odds ratio, 0.38; 95% confidence interval, 0.29 - 0.50). A weaker effect was seen in UC (allele frequency, 4.6%; odds ratio, 0.73; 95% confidence interval, 0.55-0.96). Analysis accounting for Arg381Gln suggested that other loci within IL23R also influence IBD susceptibility. Within CD, there were no subphenotype associations or evidence of interaction with CARD15. Conclusions: This study shows an association between IL23R and all sub-phenotypes of CD with a smaller effect on UC. This extends the findings of the North American study, providing clear evidence that genome-wide association scanning can successfully identify true complex disease genes

U2 - 10.1053/j.gastro.2007.02.051

DO - 10.1053/j.gastro.2007.02.051

M3 - Article

SN - 1528-0012

VL - 132

SP - 1657

EP - 1664

JO - Gastroenterology

JF - Gastroenterology

IS - 5

ER -

IL23R variation determines susceptibility but not disease phenotype in inflammatory bowel disease

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