Genetic Sequencing of Pediatric Patients Identifies Mutations in Monogenic Inflammatory Bowel Disease Genes that Translate to Distinct Clinical Phenotypes

Monogenic inflammatory bowel disease (IBD) comprises rare Mendelian causes of gut inflammation, often presenting in infants with severe and atypical disease. This study aimed to identify clinically relevant variants within 68 monogenic IBD genes in an unselected pediatric IBD cohort. METHODS: Whole...

Descripción completa

Detalles Bibliográficos
Autores principales: Ashton, James J., Mossotto, Enrico, Stafford, Imogen S., Haggarty, Rachel, Coelho, Tracy A.F., Batra, Akshay, Afzal, Nadeem A., Mort, Matthew, Bunyan, David, Beattie, Robert Mark, Ennis, Sarah
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Wolters Kluwer 2020
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7145023/
https://www.ncbi.nlm.nih.gov/pubmed/32463623
http://dx.doi.org/10.14309/ctg.0000000000000129
_version_ 1783519928779800576
author Ashton, James J.
Mossotto, Enrico
Stafford, Imogen S.
Haggarty, Rachel
Coelho, Tracy A.F.
Batra, Akshay
Afzal, Nadeem A.
Mort, Matthew
Bunyan, David
Beattie, Robert Mark
Ennis, Sarah
author_facet Ashton, James J.
Mossotto, Enrico
Stafford, Imogen S.
Haggarty, Rachel
Coelho, Tracy A.F.
Batra, Akshay
Afzal, Nadeem A.
Mort, Matthew
Bunyan, David
Beattie, Robert Mark
Ennis, Sarah
author_sort Ashton, James J.
collection PubMed
description Monogenic inflammatory bowel disease (IBD) comprises rare Mendelian causes of gut inflammation, often presenting in infants with severe and atypical disease. This study aimed to identify clinically relevant variants within 68 monogenic IBD genes in an unselected pediatric IBD cohort. METHODS: Whole exome sequencing was performed on patients with pediatric-onset disease. Variants fulfilling the American College of Medical Genetics criteria as “pathogenic” or “likely pathogenic” were assessed against phenotype at diagnosis and follow-up. Individual patient variants were assessed and processed to generate a per-gene, per-individual, deleteriousness score. RESULTS: Four hundred one patients were included, and the median age of disease-onset was 11.92 years. In total, 11.5% of patients harbored a monogenic variant. TRIM22-related disease was implicated in 5 patients. A pathogenic mutation in the Wiskott-Aldrich syndrome (WAS) gene was confirmed in 2 male children with severe pancolonic inflammation and primary sclerosing cholangitis. In total, 7.3% of patients with Crohn's disease had apparent autosomal recessive, monogenic NOD2-related disease. Compared with non-NOD2 Crohn's disease, these patients had a marked stricturing phenotype (odds ratio 11.52, significant after correction for disease location) and had undergone significantly more intestinal resections (odds ratio 10.75). Variants in ADA, FERMT1, and LRBA did not meet the criteria for monogenic disease in any patients; however, case-control analysis of mutation burden significantly implicated these genes in disease etiology. DISCUSSION: Routine whole exome sequencing in pediatric patients with IBD results in a precise molecular diagnosis for a subset of patients with IBD, providing the opportunity to personalize therapy. NOD2 status informs risk of stricturing disease requiring surgery, allowing clinicians to direct prognosis and intervention.
format Online
Article
Text
id pubmed-7145023
institution National Center for Biotechnology Information
language English
publishDate 2020
publisher Wolters Kluwer
record_format MEDLINE/PubMed
spelling pubmed-71450232020-04-17 Genetic Sequencing of Pediatric Patients Identifies Mutations in Monogenic Inflammatory Bowel Disease Genes that Translate to Distinct Clinical Phenotypes Ashton, James J. Mossotto, Enrico Stafford, Imogen S. Haggarty, Rachel Coelho, Tracy A.F. Batra, Akshay Afzal, Nadeem A. Mort, Matthew Bunyan, David Beattie, Robert Mark Ennis, Sarah Clin Transl Gastroenterol Article Monogenic inflammatory bowel disease (IBD) comprises rare Mendelian causes of gut inflammation, often presenting in infants with severe and atypical disease. This study aimed to identify clinically relevant variants within 68 monogenic IBD genes in an unselected pediatric IBD cohort. METHODS: Whole exome sequencing was performed on patients with pediatric-onset disease. Variants fulfilling the American College of Medical Genetics criteria as “pathogenic” or “likely pathogenic” were assessed against phenotype at diagnosis and follow-up. Individual patient variants were assessed and processed to generate a per-gene, per-individual, deleteriousness score. RESULTS: Four hundred one patients were included, and the median age of disease-onset was 11.92 years. In total, 11.5% of patients harbored a monogenic variant. TRIM22-related disease was implicated in 5 patients. A pathogenic mutation in the Wiskott-Aldrich syndrome (WAS) gene was confirmed in 2 male children with severe pancolonic inflammation and primary sclerosing cholangitis. In total, 7.3% of patients with Crohn's disease had apparent autosomal recessive, monogenic NOD2-related disease. Compared with non-NOD2 Crohn's disease, these patients had a marked stricturing phenotype (odds ratio 11.52, significant after correction for disease location) and had undergone significantly more intestinal resections (odds ratio 10.75). Variants in ADA, FERMT1, and LRBA did not meet the criteria for monogenic disease in any patients; however, case-control analysis of mutation burden significantly implicated these genes in disease etiology. DISCUSSION: Routine whole exome sequencing in pediatric patients with IBD results in a precise molecular diagnosis for a subset of patients with IBD, providing the opportunity to personalize therapy. NOD2 status informs risk of stricturing disease requiring surgery, allowing clinicians to direct prognosis and intervention. Wolters Kluwer 2020-02-18 /pmc/articles/PMC7145023/ /pubmed/32463623 http://dx.doi.org/10.14309/ctg.0000000000000129 Text en © 2020 The Author(s). Published by Wolters Kluwer Health, Inc. on behalf of The American College of Gastroenterology This is an open-access article distributed under the terms of the Creative Commons Attribution-Non Commercial-No Derivatives License 4.0 (CCBY-NC-ND) (http://creativecommons.org/licenses/by-nc-nd/4.0/) , where it is permissible to download and share the work provided it is properly cited. The work cannot be changed in any way or used commercially without permission from the journal.
spellingShingle Article
Ashton, James J.
Mossotto, Enrico
Stafford, Imogen S.
Haggarty, Rachel
Coelho, Tracy A.F.
Batra, Akshay
Afzal, Nadeem A.
Mort, Matthew
Bunyan, David
Beattie, Robert Mark
Ennis, Sarah
Genetic Sequencing of Pediatric Patients Identifies Mutations in Monogenic Inflammatory Bowel Disease Genes that Translate to Distinct Clinical Phenotypes
title Genetic Sequencing of Pediatric Patients Identifies Mutations in Monogenic Inflammatory Bowel Disease Genes that Translate to Distinct Clinical Phenotypes
title_full Genetic Sequencing of Pediatric Patients Identifies Mutations in Monogenic Inflammatory Bowel Disease Genes that Translate to Distinct Clinical Phenotypes
title_fullStr Genetic Sequencing of Pediatric Patients Identifies Mutations in Monogenic Inflammatory Bowel Disease Genes that Translate to Distinct Clinical Phenotypes
title_full_unstemmed Genetic Sequencing of Pediatric Patients Identifies Mutations in Monogenic Inflammatory Bowel Disease Genes that Translate to Distinct Clinical Phenotypes
title_short Genetic Sequencing of Pediatric Patients Identifies Mutations in Monogenic Inflammatory Bowel Disease Genes that Translate to Distinct Clinical Phenotypes
title_sort genetic sequencing of pediatric patients identifies mutations in monogenic inflammatory bowel disease genes that translate to distinct clinical phenotypes
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7145023/
https://www.ncbi.nlm.nih.gov/pubmed/32463623
http://dx.doi.org/10.14309/ctg.0000000000000129
work_keys_str_mv AT ashtonjamesj geneticsequencingofpediatricpatientsidentifiesmutationsinmonogenicinflammatoryboweldiseasegenesthattranslatetodistinctclinicalphenotypes
AT mossottoenrico geneticsequencingofpediatricpatientsidentifiesmutationsinmonogenicinflammatoryboweldiseasegenesthattranslatetodistinctclinicalphenotypes
AT staffordimogens geneticsequencingofpediatricpatientsidentifiesmutationsinmonogenicinflammatoryboweldiseasegenesthattranslatetodistinctclinicalphenotypes
AT haggartyrachel geneticsequencingofpediatricpatientsidentifiesmutationsinmonogenicinflammatoryboweldiseasegenesthattranslatetodistinctclinicalphenotypes
AT coelhotracyaf geneticsequencingofpediatricpatientsidentifiesmutationsinmonogenicinflammatoryboweldiseasegenesthattranslatetodistinctclinicalphenotypes
AT batraakshay geneticsequencingofpediatricpatientsidentifiesmutationsinmonogenicinflammatoryboweldiseasegenesthattranslatetodistinctclinicalphenotypes
AT afzalnadeema geneticsequencingofpediatricpatientsidentifiesmutationsinmonogenicinflammatoryboweldiseasegenesthattranslatetodistinctclinicalphenotypes
AT mortmatthew geneticsequencingofpediatricpatientsidentifiesmutationsinmonogenicinflammatoryboweldiseasegenesthattranslatetodistinctclinicalphenotypes
AT bunyandavid geneticsequencingofpediatricpatientsidentifiesmutationsinmonogenicinflammatoryboweldiseasegenesthattranslatetodistinctclinicalphenotypes
AT beattierobertmark geneticsequencingofpediatricpatientsidentifiesmutationsinmonogenicinflammatoryboweldiseasegenesthattranslatetodistinctclinicalphenotypes
AT ennissarah geneticsequencingofpediatricpatientsidentifiesmutationsinmonogenicinflammatoryboweldiseasegenesthattranslatetodistinctclinicalphenotypes

Ejemplares similares