For simplicity, we refer to these disorders in the following text as monogenic IBD, even if there is a spectrum of penetrance of the IBD phenotype. We will compare those monogenic forms of IBD with polygenic conventional IBD. All data suggest that the fraction of monogenic disorders with IBD-like presentation among ICG-001 supplier all patients with IBD correlates inversely with the age of onset. Despite a growing genotype spectrum, monogenic disorders still account for only a fraction of VEOIBD cases. The true fraction is unknown. In a study of 66 patients who developed IBD at ages younger than 5 years, 5 patients were found to carry mutations
in IL10RA, 8 in IL10RB, and 3 in IL10. 30 All patients developed symptoms within the first
3 months of life. 30 A recent study detected 4 patients with presumed pathogenic XIAP mutations in a group of 275 patients with pediatric IBD (A1a/A1b Paris classification) and 1047 patients with adult-onset CD (A2 and A3 Montreal classification). 31 Because all patients with XIAP variants were infantile to adolescent male patients with CD, this could suggest an approximate prevalence of 4% among young male patients with IBD. However, studies like these focus on specific genes and may have strong selection bias toward an expected clinical subphenotype. They might therefore overestimate Rebamipide the frequency of specific variants. GSK2118436 clinical trial Analysis of large, multicenter, population-based cohorts is needed to determine the proportion of cases of VEOIBD caused by single gene defects and to estimate penetrance. Monogenic defects have been found to alter intestinal immune homeostasis via several mechanisms (Table 2). These include disruption of the epithelial barrier and the epithelial response as well as reduced clearance of bacteria by neutrophil granulocytes and other phagocytes. Other single-gene defects induce hyperinflammation or autoinflammation or disrupt T- and B-cell selection and activation. Hyperactivation of the
immune response can result from defects in immune inhibitory mechanisms, such as defects in IL-10 signaling or dysfunctional regulatory T-cell activity. Genetic disorders that affect intestinal epithelial barrier function include dystrophic epidermolysis bullosa,32 Kindler syndrome,32 familial diarrhea caused by dominant activating mutations in guanylate cyclase C,33 X-linked ectodermal dysplasia and immunodeficiency,34 and ADAM17 deficiency.35 X-linked ectodermal dysplasia and immunodeficiency, caused by hypomorphic mutations in IKBKG (encodes nuclear factor κB essential modulator protein [NEMO]) 34 and ADAM17 deficiency 35 cause epithelial and immune dysfunction.