Your search keyword '"Fisher, Sheila A."' showing total 13 results

1. Common variants at five new loci associated with early-onset inflammatory bowel disease.

Author

Imielinski M, Baldassano RN, Griffiths A, Russell RK, Annese V, Dubinsky M, Kugathasan S, Bradfield JP, Walters TD, Sleiman P, Kim CE, Muise A, Wang K, Glessner JT, Saeed S, Zhang H, Frackelton EC, Hou C, Flory JH, Otieno G, Chiavacci RM, Grundmeier R, Castro M, Latiano A, Dallapiccola B, Stempak J, Abrams DJ, Taylor K, McGovern D, Silber G, Wrobel I, Quiros A, Barrett JC, Hansoul S, Nicolae DL, Cho JH, Duerr RH, Rioux JD, Brant SR, Silverberg MS, Taylor KD, Barmuda MM, Bitton A, Dassopoulos T, Datta LW, Green T, Griffiths AM, Kistner EO, Murtha MT, Regueiro MD, Rotter JI, Schumm LP, Steinhart AH, Targan SR, Xavier RJ, Libioulle C, Sandor C, Lathrop M, Belaiche J, Dewit O, Gut I, Heath S, Laukens D, Mni M, Rutgeerts P, Van Gossum A, Zelenika D, Franchimont D, Hugot JP, de Vos M, Vermeire S, Louis E, Cardon LR, Anderson CA, Drummond H, Nimmo E, Ahmad T, Prescott NJ, Onnie CM, Fisher SA, Marchini J, Ghori J, Bumpstead S, Gwillam R, Tremelling M, Delukas P, Mansfield J, Jewell D, Satsangi J, Mathew CG, Parkes M, Georges M, Daly MJ, Heyman MB, Ferry GD, Kirschner B, Lee J, Essers J, Grand R, Stephens M, Levine A, Piccoli D, Van Limbergen J, Cucchiara S, Monos DS, Guthery SL, Denson L, Wilson DC, Grant SF, Daly M, Silverberg MS, Satsangi J, and Hakonarson H

Subjects

Age of Onset, Chromosome Mapping, Colitis, Ulcerative genetics, Genome, Human, Genome-Wide Association Study, Humans, Inflammatory Bowel Diseases epidemiology, Genetic Variation, Inflammatory Bowel Diseases genetics

Abstract

The inflammatory bowel diseases (IBD) Crohn's disease and ulcerative colitis are common causes of morbidity in children and young adults in the western world. Here we report the results of a genome-wide association study in early-onset IBD involving 3,426 affected individuals and 11,963 genetically matched controls recruited through international collaborations in Europe and North America, thereby extending the results from a previous study of 1,011 individuals with early-onset IBD. We have identified five new regions associated with early-onset IBD susceptibility, including 16p11 near the cytokine gene IL27 (rs8049439, P = 2.41 x 10(-9)), 22q12 (rs2412973, P = 1.55 x 10(-9)), 10q22 (rs1250550, P = 5.63 x 10(-9)), 2q37 (rs4676410, P = 3.64 x 10(-8)) and 19q13.11 (rs10500264, P = 4.26 x 10(-10)). Our scan also detected associations at 23 of 32 loci previously implicated in adult-onset Crohn's disease and at 8 of 17 loci implicated in adult-onset ulcerative colitis, highlighting the close pathogenetic relationship between early- and adult-onset IBD.

Published

2009

2. Combined evidence from three large British Association studies rejects TUCAN/CARD8 as an IBD susceptibility gene.

Author

Fisher SA, Mirza MM, Onnie CM, Soars D, Lewis CM, Prescott NJ, Mathew CG, Sanderson J, Forbes A, Todhunter C, Donaldson P, and Mansfield J

Subjects

CARD Signaling Adaptor Proteins physiology, Cohort Studies, England, Frameshift Mutation genetics, Humans, Inflammatory Bowel Diseases physiopathology, Neoplasm Proteins physiology, CARD Signaling Adaptor Proteins genetics, Genetic Predisposition to Disease, Inflammatory Bowel Diseases genetics, Neoplasm Proteins genetics

Published

2007

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

Author

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, and Satsangi J

Subjects

Adult, Case-Control Studies, Cohort Studies, Colitis, Ulcerative genetics, Colitis, Ulcerative pathology, Crohn Disease genetics, Crohn Disease pathology, England, Epistasis, Genetic, Female, Humans, Inflammatory Bowel Diseases pathology, Male, Nod2 Signaling Adaptor Protein genetics, Risk Factors, Scotland, Genetic Predisposition to Disease genetics, Inflammatory Bowel Diseases genetics, Phenotype, Polymorphism, Single Nucleotide genetics, Receptors, Interleukin genetics

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 chi(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(-12)]; 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 subphenotypes 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.

Published

2007

4. Investigation of association of the DLG5 gene with phenotypes of inflammatory bowel disease in the British population.

Author

Pearce AV, Fisher SA, Prescott NJ, Onnie CM, Pattni R, Green P, Forbes A, Mansfield J, Sanderson J, Schreiber S, Lewis CM, and Mathew CG

Subjects

Case-Control Studies, Cohort Studies, Colitis, Ulcerative genetics, Crohn Disease genetics, England, Gene Frequency, Genetic Predisposition to Disease, Genotype, Humans, Inflammatory Bowel Diseases epidemiology, Inflammatory Bowel Diseases etiology, Phenotype, Smoking, Inflammatory Bowel Diseases genetics, Membrane Proteins genetics, Polymorphism, Genetic, Tumor Suppressor Proteins genetics

Abstract

Background and Aims: Mutations in the DLG5 gene are associated with an increased risk of inflammatory bowel disease (IBD) in some European populations. Initial investigation of a British IBD population showed evidence of association of one of three DLG5 variants, R30Q, in a family-based collection but not in a case-control cohort. We have now examined the association of the R30Q polymorphism in a large cohort of British IBD cases, tested for interaction between the DLG5 and CARD15 genes and assessed possible association of DLG5 with clinical features of Crohn's disease (CD) and ulcerative colitis (UC)., Materials and Methods: DLG5 R30Q and the CARD15 polymorphisms, Arg702Trp, Gly908Arg and Leu1007fs were genotyped in 1,148 IBD cases and 749 controls. DLG5 R30Q was also analysed in cases stratified by CARD15 genotype, disease subtype and smoking history., Results/findings: No significant difference in frequencies of the R30Q variant was observed between IBD cases (9.9%) and controls (10.1%) or in cases analysed separately as CD and UC. There was also no significant difference in the frequency of R30Q between CD cases carrying risk-associated CARD15 alleles and those that did not. The frequency of R30Q was higher in CD cases with ileal disease than cases without (p=0.042) and higher in CD cases who had smoked than in nonsmokers (p=0.009)., Interpretation/conclusion: The R30Q variant in the DLG5 gene does not appear to be associated with an overall increase in the risk of disease in a British IBD cohort, but differences in its frequency in subgroups of CD patients warrant further investigation.

Published

2007

5. Associations of allelic variants of the multidrug resistance gene (ABCB1 or MDR1) and inflammatory bowel disease and their effects on disease behavior: a case-control and meta-analysis study.

Author

Onnie CM, Fisher SA, Pattni R, Sanderson J, Forbes A, Lewis CM, and Mathew CG

Subjects

ATP Binding Cassette Transporter, Subfamily B, Adolescent, Adult, Aged, Aged, 80 and over, Alleles, Child, Child, Preschool, Disease Progression, Female, Follow-Up Studies, Genotype, Humans, Inflammatory Bowel Diseases genetics, Male, Middle Aged, Retrospective Studies, ATP Binding Cassette Transporter, Subfamily B, Member 1 genetics, DNA genetics, Gene Frequency, Inflammatory Bowel Diseases metabolism, Organic Anion Transporters genetics, Polymorphism, Genetic

Abstract

Background: Allelic variants of the ATP-binding cassette, subfamily B member 1 (ABCB1), also known as the multidrug resistance gene (MDR1) that encodes the membrane-bound efflux transporter P-glycoprotein 170 (PGP-170), have been associated with inflammatory bowel disease but with conflicting results., Methods: The present study examined the association of ABCB1 C3435T and G2677T/A in a large British case-control cohort of 828 Crohn's disease, 580 ulcerative colitis (UC) cases, and 285 healthy controls. The effect of these variants was further examined with respect to phenotypic and epidemiological characteristics. A meta-analysis was carried out of our results and those from 8 previously published association studies of the C3435T variant in inflammatory bowel disease., Results: The 2677T allele was significantly increased in British UC cases compared with controls (45.2% vs. 39.6%; P = 0.034). In particular, the TT genotype was significantly associated with severe UC (odds ratio [OR] 1.90; 95% CI 1.01-3.55) and the use of steroids in UC (OR 1.77; 95% CI 1.08-2.88). No significant association was seen with C3435T and UC, Crohn's disease, or any clinical subgroup. A meta-analysis of 9 association studies of C3435T showed a significant association of the 3435T allele with UC (OR 1.12; 95% CI 1.02-1.23; P = 0.013) but not with CD., Conclusions: These results indicate that ABCB1 sequence variants are associated with a small increase in the risk of developing UC and may influence disease behavior.

Published

2006

6. Association of DLG5 R30Q variant with inflammatory bowel disease.

Author

Daly MJ, Pearce AV, Farwell L, Fisher SA, Latiano A, Prescott NJ, Forbes A, Mansfield J, Sanderson J, Langelier D, Cohen A, Bitton A, Wild G, Lewis CM, Annese V, Mathew CG, and Rioux JD

Subjects

Case-Control Studies, Colitis, Ulcerative genetics, Crohn Disease genetics, Humans, Polymorphism, Single Nucleotide, Quebec, United Kingdom, Genetic Predisposition to Disease, Genetic Variation, Inflammatory Bowel Diseases genetics, Membrane Proteins genetics, Tumor Suppressor Proteins genetics

Abstract

Crohn's disease (CD) and ulcerative colitis (UC) are chronic inflammatory diseases of the gastrointestinal system known as the inflammatory bowel diseases (IBD). Recently, Stoll and colleagues reported a novel finding of genetic variation in the DLG5 gene that is associated with IBD (CD and UC combined). We present here a study of the genetic variation described in that report in two well-powered, independent case-control cohorts and one family-based collection, and confirm the proposed association between IBD and the R30Q variant of DLG5 in two of the three studies. We are, however, unable to replicate the other proposed association to the common haplotype described in Stoll et al and suggest that this other finding could conceivably have been partially a statistical fluctuation and partially a result of LD with the replicated R30Q association. This study provides support for the hypothesis that DLG5 constitutes a true IBD risk factor of modest effect.

Published

2005

7. Inflammatory bowel disease susceptibility loci defined by genome scan meta-analysis of 1952 affected relative pairs.

Author

van Heel DA, Fisher SA, Kirby A, Daly MJ, Rioux JD, and Lewis CM

Subjects

Chromosomes ultrastructure, Colitis, Ulcerative genetics, Crohn Disease genetics, Genetic Linkage, Humans, Mutation, Phenotype, Statistics as Topic, Genetic Predisposition to Disease, Genome, Human, Inflammatory Bowel Diseases genetics

Abstract

Crohn's disease and ulcerative colitis (the inflammatory bowel diseases) have a strong genetic component. Although over 20 putative susceptibility loci have been identified by individual genome scans, the majority of these loci have not been replicated. Many individual studies are at the lower limit of acceptable power for complex disease linkage analysis. Genome scan meta-analysis (GSMA), by use of sample sizes an order of magnitude greater than individual linkage studies, has increased power to detect novel loci, may confirm or refute regions detected in smaller individual studies, and enables regions to be prioritized for further gene identification efforts. Genome scan data (markers, significance scores) were obtained from 10 separate studies and meta-analysis was performed using the GSMA method. These studies comprised 1952 inflammatory bowel disease, 1068 Crohn's disease and 457 ulcerative colitis affected relative pairs. Study results were divided into 34 cM chromosomal bins, ranked, weighted by study size, summed across studies and bin-by-bin significance obtained by simulation. A region on chromosome 6p (containing the HLA) met genome wide significance for inflammatory bowel disease. Loci meeting suggestive significance for inflammatory bowel disease were 2q, 3q, 5q, 7q and 16 (NOD2/CARD15 region); Crohn's disease, 2q, 3q, 6p, 16 (NOD2/CARD15 region), 17q, 19p; and ulcerative colitis, 2q. Clustering of adjacent bins was observed for chromosomes 6p, 16, 19p. The meta-analysis has identified novel loci and prioritized genomic regions for further gene identification studies.

Published

2004

8. Sex stratification of an inflammatory bowel disease genome search shows male-specific linkage to the HLA region of chromosome 6.

Author

Fisher SA, Hampe J, Macpherson AJ, Forbes A, Lennard-Jones JE, Schreiber S, Curran ME, Mathew CG, and Lewis CM

Subjects

Chromosome Mapping, Colitis, Ulcerative genetics, Crohn Disease genetics, Female, Genetic Markers, Humans, Lod Score, Male, Nuclear Family, Chromosomes, Human, Pair 6 genetics, Genetic Linkage, Genetic Predisposition to Disease, HLA Antigens genetics, Inflammatory Bowel Diseases genetics, Sex Characteristics

Abstract

Inflammatory bowel disease (IBD) is a multifactorial disorder, with both genetic and environmental factors contributing to the two clinical phenotypes of Crohn's disease (CD) and ulcerative colitis (UC). The underlying genetic model is thought to involve multiple genes with complex interactions between disease loci, and the NOD2 gene on chromosome 16 has recently been identified as a CD susceptibility locus. Several genome-wide linkage studies have identified candidate regions, but there has been little replication across studies. Here we investigate the role of sex-specific loci in susceptibility to IBD. Linkage data from our previously reported genome search and follow-up study were stratified by the sex of the affected sib pair. Non-parametric linkage analysis was performed using Genehunter Plus. Simulation studies were used to assess the significance of differences in LOD scores between male and female families for each chromosome. Several regions of sex-specific linkage were identified, including existing and novel candidate loci. The major histocompatibility region on chromosome 6p, referred to as IBD3, showed evidence of male-specific linkage with a maximum LOD score of 5.9 in both CD and UC male-affected families. Regions on chromosomes 11, 14 and 18 showed strong evidence of linkage in male-affected families but not in female-affected families. No evidence of sex-specific linkage was found in the IBD1 or IBD2 candidate regions of chromosomes 16 and 12. The existence of sex-specific linkage is further evidence of the complex mechanisms involved in IBD and will facilitate future studies to identify susceptibility genes.

Published

2002

9. Investigation of Crohn's Disease Risk Loci in Ulcerative Colitis Further Defines Their Molecular Relationship.

Author

Anderson, Carl A., Massey, Dunecan C.O., Barrett, Jeffrey C., Prescott, Natalie J., Tremelling, Mark, Fisher, Sheila A., Gwilliam, Rhian, Jacob, Jemima, Nimmo, Elaine R., Drummond, Hazel, Lees, Charlie W., Onnie, Clive M., Hanson, Catherine, Blaszczyk, Katarzyna, Ravindrarajah, Radhi, Hunt, Sarah, Varma, Dhiraj, Hammond, Naomi, Lewis, Gregory, and Attlesey, Heather

Subjects

CROHN'S disease, ULCERATIVE colitis, INFLAMMATORY bowel diseases, GENETIC polymorphisms, CHROMOSOMES, META-analysis, GENETICS of disease susceptibility, GENETICS, DISEASE risk factors

Abstract

Background & Aims: Identifying shared and disease-specific susceptibility loci for Crohn''s disease (CD) and ulcerative colitis (UC) would help define the biologic relationship between the inflammatory bowel diseases. More than 30 CD susceptibility loci have been identified. These represent important candidate susceptibility loci for UC. Loci discovered by the index genome scans in CD have previously been tested for association with UC, but those identified in the recent meta-analysis await such investigation. Furthermore, the recently identified UC locus at ECM1 requires formal testing for association with CD. Methods: We analyzed 45 single nucleotide polymorphisms, tagging 29 of the loci recently associated with CD in 2527 UC cases and 4070 population controls. We also genotyped the UC-associated ECM1 variant rs11205387 in 1560 CD patients and 3028 controls. Results: Nine regions showed association with UC at a threshold corrected for the 29 loci tested (P < .0017). The strongest association (P = 4.13 × 10−8; odds ratio = 1.27) was identified with a 170-kilobase region on chromosome 1q32 that contains 3 genes. We also found association with JAK2 and replicated a recently reported association with STAT3, further implicating the role of this signaling pathway in inflammatory bowel disease. Additional novel UC susceptibility genes were LYRM4 and CDKAL1. Twenty of the loci were not associated with UC, and several appear to be specific to CD. ECM1 variation was not associated with CD. Conclusions: Collectively, these data help define the genetic relationship between CD and UC and characterize common, as well as disease-specific mechanisms of pathogenesis. [Copyright &y& Elsevier]

Published

2009

10. A Nonsynonymous SNP in ATG16L1 Predisposes to Ileal Crohn’s Disease and Is Independent of CARD15 and IBD5.

Author

Prescott, Natalie J., Fisher, Sheila A., Franke, Andre, Hampe, Jochen, Onnie, Clive M., Soars, Dianne, Bagnall, Richard, Mirza, Muddassar M., Sanderson, Jeremy, Forbes, Alastair, Mansfield, John C., Lewis, Cathryn M., Schreiber, Stefan, and Mathew, Christopher G.

Subjects

INFLAMMATORY bowel diseases, ULCERATIVE colitis, INTESTINAL diseases, GENETICS of disease susceptibility

Abstract

Background & Aims: A genome-wide association scan of nonsynonymous DNA polymorphisms identified association of a threonine-to-alanine substitution (T300A) in the autophagy-related 16-like gene ATG16L1 with Crohn’s disease. We investigated this association in independent U.K. cohorts of Crohn’s disease and ulcerative colitis. Methods: The T300A variant (rs2241880) was genotyped in an independent sample of 727 Crohn’s disease and 877 ulcerative colitis cases, and in 579 controls. We then performed an extension analysis combining these data with the U.K. data from the initial study to give a total of 1236 U.K. Crohn’s disease cases and 1235 controls to estimate disease risk and test for interaction with the CARD15 and IBD5 risk loci and for association with disease subtypes. Results: The association of T300A was replicated in the independent sample of 727 Crohn’s disease cases (P = .001), and was strongly associated in the extended analysis of 1236 Crohn’s cases (P = 2.4 × 10−6). The 300A/A genotype conferred a 1.65-fold risk of Crohn’s disease, with a 2.2-fold risk of ileal disease. Analysis of the interaction of ATG16L1 with CARD15 and IBD5 indicated that all 3 loci contribute independently to disease risk. Homozygosity for the risk allele at all 3 loci conferred a combined risk of 20.4 (95% confidence interval: 8.71, 47.7) for Crohn’s disease. The ATG16L1 risk genotype showed a modest but significant association with ulcerative colitis (P = .026). Conclusions: The association of ATG16L1 with Crohn’s disease and possibly with ulcerative colitis supports a role for autophagy in the pathogenesis of inflammatory bowel disease. [Copyright &y& Elsevier]

Published

2007

11. Genetic determinants of ulcerative colitis include the ECM1 locus and five loci implicated in Crohn's disease.

Author

Fisher, Sheila A., Tremelling, Mark, Anderson, Carl A, Gwilliam, Rhian, Bumpstead, Suzannah, Prescott, Natalie J., Nimmo, Elaine R., Massey, Dunecan, Berzuini, Carlo, Johnson, Christopher, Barrett, Jeffrey C., Cummings, Fraser R., Drummond, Hazel, Lees, Charlie W., Onnie, Clive M., Hanson, Catherine E., Blaszczyk, Katarzyna, Inouye, Mike, Ewels, Philip, and Ravindrarajah, Radhi

Subjects

*HUMAN genetics, *ULCERATIVE colitis, *CROHN'S disease, *INFLAMMATORY bowel diseases, *INTESTINAL diseases

Abstract

We report results of a nonsynonymous SNP scan for ulcerative colitis and identify a previously unknown susceptibility locus at ECM1. We also show that several risk loci are common to ulcerative colitis and Crohn's disease (IL23R, IL12B, HLA, NKX2-3 and MST1), whereas autophagy genes ATG16L1 and IRGM, along with NOD2 (also known as CARD15), are specific for Crohn's disease. These data provide the first detailed illustration of the genetic relationship between these common inflammatory bowel diseases. [ABSTRACT FROM AUTHOR]

Published

2008

12. Identification, evolution, and association study of a novel promoter and first exon of the human NOD2 (CARD15) gene

Author

King, Kathy, Bagnall, Richard, Fisher, Sheila A., Sheikh, Faisal, Cuthbert, Andrew, Tan, Sipin, Mundy, Nicholas I., Rosenstiel, Philip, Schreiber, Stefan, Mathew, Christopher G., and Roberts, Roland G.

Subjects

*CROHN'S disease, *INFLAMMATORY bowel diseases, *GASTROENTERITIS, *INFLAMMATION

Abstract

Abstract: Mutations in the NOD2 (CARD15) gene predispose to Crohn''s disease (CD), a human chronic inflammatory bowel disorder, and can cause Blau syndrome. During an investigation of an apparent correlation between a frameshifting mutation in the canonical first exon of NOD2 of marmoset and tamarin species and their susceptibility to chronic colitis, we found that, contrary to previous reports, the basal levels of NOD2 transcripts in tissues relevant to CD arise from a distinct novel promoter and first exon. The canonical first exon, by contrast, seems to be of negligible transcriptional importance under physiological conditions, and its reading frame has been disrupted twice during primate evolution. Thus the main NOD2/CARD15 protein isoform produced in humans and other primates is 27 amino acids shorter than previously reported, starting at a conserved methionine in exon 2. We show that there is no significant association between variants in the novel NOD2 promoter region and CD. [Copyright &y& Elsevier]

Published

2007

13. Association between insertion mutation in NOD2 gene and Crohn's disease in German and British populations.

Author

Hampe, Jochen, Cuthbert, Andrew, Croucher, Peter J P, Mirza, Muddassar M, Mascheretti, Silvia, Fisher, Sheila, Frenzel, Henning, King, Kathy, Hasselmeyer, Anja, MacPherson, Andrew J S, Bridger, Stephen, van Deventer, Sander, Forbes, Alastair, Nikolaus, Susanna, Lennard-Jones, John E, Foelsch, Ulrich R, Krawczak, Michael, Lewis, Cathryn, Schreiber, Stefan, and Mathew, Christopher G

Subjects

*INFLAMMATORY bowel diseases, *GENETICS of Crohn's disease, *GENETIC mutation, *DISEASE susceptibility, *GENETICS

Abstract

Background Genetic predisposition to inflammatory bowel disease (IBD) has been shown by epidemiological and linkage studies. Genetic linkage of IBD to chromosome 16 has been previously observed and replicated in independent populations. The recently identified NOD2 gene is a good positional and functional candidate gene since it is located in the region of linkage on chromosome 16q12, and activates nuclear factor (NF) kappaB in response to bacterial lipopolysaccharides. Methods We sequenced the coding region of the NOD2 gene and genotyped an insertion polymorphism affecting the leucine-rich region of the protein product in 512 individuals with IBD from 309 German or British families, 369 German trios (ie, German patients with sporadic IBD and their unaffected parents), and 272 normal controls. We then tested for association with Crohn's disease and ulcerative colitis. Findings Family-based association analyses were consistently positive in 95 British and 99 German affected sibling pairs with Crohn's disease (combined p<0.0001); the association was confirmed in the 304 German trios with Crohn's disease. No association was seen in the 115 sibling pairs and 65 trios with ulcerative colitis. The genotype-specific disease risks conferred by heterozygous and homozygous mutant genotypes were 2.6 (95% CI 1.5-4.5) and 42.1 (4.3-infinity), respectively. Interpretation The insertion mutation in the NOD2 gene confers a substantially increased susceptibility to Crohn's disease but not to ulcerative colitis. [ABSTRACT FROM AUTHOR]

Published

2001