Influence of a nucleotide oligomerization domain 1 (NOD1) polymorphism and NOD2 mutant alleles on Crohn's disease phenotype

被引:19
作者
Canto, Elisabet
Ricart, Elena
Busquets, David
Monfort, David
Garcia-Planella, Esther
Gonzalez, Dolors
Balanzo, Joaquim
Rodriguez-Sanchez, Jose L.
Vidal, Silvia
机构
[1] St Pau Hosp, Dept Immunol, St Pau Hosp & Res Inst, Inst Rec, Barcelona 08025, Spain
[2] Clin Hosp, CIBER EHD, Dept Gastroenterol, Barcelona 08025, Spain
[3] St Pau Hosp, Dept Digest Pathol, Barcelona 08025, Spain
关键词
Crohn's disease; nucleotide oligomerization domain 1; nucleotide oligomerization domain 2;
D O I
10.3748/wjg.v13.i41.5446
中图分类号
R57 [消化系及腹部疾病];
学科分类号
摘要
AIM: To examine genetic variation of nucleoticle oligomerization domain 1 (NODI) and NOD2, their respective influences on Crohn's disease phenotype and gene-gene interactions. METHODS: (ND1+32656*1) NODI polymorphism and SNP8, 5NP12 and SNP13 of NOD2 were analyzed in 97 patients and 50 controls. NOD2 variants were determined by reaction restriction fragment length polymorphism analysis. NODI genotyping and NOD2 variant confirmation were performed by specific amplification and sequencing. RESULTS: The distribution of NODI polymorphism in patients was different from controls (P = 0.045) and not altered by existence of NOD2 mutations. In this cohort, 30.92% patients and 6% controls carried at least one NOD2 variant (P < 0.001) with R702W being the most frequent variant. Presence of at least one NOD2 mutation was inversely associated with colon involvement (9.09% with colon vs 36.4% with ileal or ileocolonic involvement, P = 0.04) and indicative of risk of penetrating disease (52.63% with penetrating vs 25.64% with non-penetrating or stricturing behavior, P = 0.02). L1007finsC and double NOD2 mutationconferred the highest risk for severity of disease (26.3% with penetrating disease vs 3.8% with non-penetrating or stricturing behavior presented L1007finsC, P = 0.01 and 21.0% with penetrating disease vs 2.5% with nonpenentrating or stricturing behavior carried double NOD2 mutation, P = 0.007). Exclusion of patients with NOD2 mutations from phenotype/NOD1 -genotype analysis revealed higher prevalence of *1*1 genotype in groups of younger age at onset and colonic location. CONCLUSION: This study suggests population differences in the inheritance of risk NOD1 polymorphism and NOD2 mutations. Although no interaction between NOD1-NOD2 was noticed, a relationship between disease location and Nod-like receptor molecules was established. (C) 2007 WJG. All rights reserved.
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页码:5446 / 5453
页数:8
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