Somatic mosaicism and common genetic variation contribute to the risk of very-early-onset inflammatory bowel disease.

Very-early-onset inflammatory bowel disease (VEO-IBD) is a heterogeneous phenotype associated with a spectrum of rare Mendelian disorders. Here, we perform whole-exome-sequencing and genome-wide genotyping in 145 patients (median age-at-diagnosis of 3.5 years), in whom no Mendelian disorders were clinically suspected. In five patients we detect a primary immunodeficiency or enteropathy, with clinical consequences (XIAP, CYBA, SH2D1A, PCSK1). We also present a case study of a VEO-IBD patient with a mosaic de novo, pathogenic allele in CYBB. The mutation is present in ~70% of phagocytes and sufficient to result in defective bacterial handling but not life-threatening infections. Finally, we show that VEO-IBD patients have, on average, higher IBD polygenic risk scores than population controls (99 patients and 18,780 controls; P < 4 × 10-10), and replicate this finding in an independent cohort of VEO-IBD cases and controls (117 patients and 2,603 controls; P < 5 × 10-10). This discovery indicates that a polygenic component operates in VEO-IBD pathogenesis.

Keywords

Adult, Age of Onset, Case-Control Studies, Child, Child, Preschool, Cohort Studies, Female, Genes, Recessive, Genetic Predisposition to Disease, Genetic Variation, Humans, Infant, Infant, Newborn, Inflammatory Bowel Diseases, Loss of Function Mutation, Male, Mosaicism, Multifactorial Inheritance, Mutation, NADPH Oxidase 2, Pedigree, Primary Immunodeficiency Diseases, Risk Factors, Exome Sequencing

Journal Title

Nat Commun

Journal ISSN

2041-1723
2041-1723

Volume Title

11

Publisher

Springer Science and Business Media LLC

Publisher DOI

https://doi.org/10.1038/s41467-019-14275-y

Rights

Sponsorship

Medical Research Council (MR/M00533X/1)
National Association for Colitis and Crohn's Disease (NACC) (MR/M00533X/1)

We thank all individuals who contributed samples to the study. We acknowledge Satish Keshav who sadly died during the revision process of this manuscript and who was instrumental to setup the Oxford IBD cohort study. The COLORS in IBD project was supported by an ESPGHAN collaboration network grant and Crohn’s and Colitis UK (M/11/01). The genotyping and sequencing of the COLORS in IBD cohort was funded by the Wellcome Trust (098051; 093885/Z/10/Z). Adult-onset IBD case collections were supported by Crohn’s and Colitis UK and sequencing was co-funded by the Wellcome Trust (098051) and the Medical Research Council, UK (MR/J00314X/1). We thank the investigators of the NIDDK IBD Genetics Consortium for sharing previously unpublished genotype data for a large cohort of population controls, used in our polygenic risk analyses. We acknowledge support of the Wellcome Trust (EGS, LM, LF, JM, JCB and CAA: 098051), the Crohn’s & Colitis Foundation of America (H.H.U), the Leona M. and Harry B. Helmsley Charitable Trust (HHU, AM, SS), the Deutsche Forschungsgemeinschaft (TS), the Swiss National Science Foundation (CPB), the Medical Research Council (AA, TAF, DCW), the Medical Research Foundation (DCW) and the Ovarian Cancer Action (AA). TAB is supported by a Radcliffe Department of Medicine/MRC Scholars Programme Studentship. The NIDDK IBD Genetics Consortium is supported by National Institute of Diabetes and Digestive and Kidney Diseases grants. We acknowledge the contribution of the Oxford Biomedical Research Centre, which is supported by the National Institute for Health Research. We thank the INTERVAL Study for contributing sequencing data. INTERVAL was supported by: NHSBT, NIHR, NIHR BioResource, NIHR [Cambridge Biomedical Research Centre at the Cambridge University Hospitals NHS Foundation Trust] [*], NIHR BTRU in Donor Health and Genomics, UK MRC, BHF, Wellcome Trust and the ESRC." J.D. is funded by the NIHR [Senior Investigator Award]. *The views expressed are those of the authors and not necessarily those of the NHS, the NIHR or the Department of Health and Social Care.

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