Exome sequencing in patient‐parent trios suggests new candidate genes for early‐onset primary sclerosing cholangitis

BACKGROUND & AIMS Primary sclerosing cholangitis (PSC) is a rare bile duct disease strongly associated with inflammatory bowel disease (IBD). Whole‐exome sequencing (WES) has contributed to understanding the molecular basis of very early‐onset IBD, but rare protein‐altering genetic variants have...

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Published in	Liver international Vol. 41; no. 5; pp. 1044 - 1057
Main Authors	Haisma, Sjoukje‐Marije, Weersma, Rinse K., Joosse, Maria E., Koning, Barbara A. E., Meij, Tim, Koot, Bart G. P., Wolters, Victorien, Norbruis, Obbe, Daly, Mark J., Stevens, Christine, Xavier, Ramnik J., Koskela, Jukka, Rivas, Manuel A., Visschedijk, Marijn C., Verkade, Henkjan J., Barbieri, Ruggero, Jansen, Dianne B. H., Festen, Eleonora A. M., Rheenen, Patrick F., Diemen, Cleo C.
Format	Journal Article
Language	English
Published	United States Wiley Subscription Services, Inc 01.05.2021 John Wiley and Sons Inc
Subjects	Algorithms Bile ducts Cholangitis Deoxyribonucleic acid DNA Gene expression Gene frequency Genes genetic Genetic diversity Genetic variance Genetics and Rare Liver Diseases Heredity Inflammatory bowel disease Inflammatory bowel diseases Innate immunity Intestine Original Pathogenicity Pathogens sclerosing cholangitis genetic inflammatory bowel disease sclerosing cholangitis
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Abstract	BACKGROUND & AIMS Primary sclerosing cholangitis (PSC) is a rare bile duct disease strongly associated with inflammatory bowel disease (IBD). Whole‐exome sequencing (WES) has contributed to understanding the molecular basis of very early‐onset IBD, but rare protein‐altering genetic variants have not been identified for early‐onset PSC. We performed WES in patients diagnosed with PSC ≤ 12 years to investigate the contribution of rare genetic variants to early‐onset PSC. METHODS In this multicentre study, WES was performed on 87 DNA samples from 29 patient‐parent trios with early‐onset PSC. We selected rare (minor allele frequency < 2%) coding and splice‐site variants that matched recessive (homozygous and compound heterozygous variants) and dominant (de novo) inheritance in the index patients. Variant pathogenicity was predicted by an in‐house developed algorithm (GAVIN), and PSC‐relevant variants were selected using gene expression data and gene function. RESULTS In 22 of 29 trios we identified at least 1 possibly pathogenic variant. We prioritized 36 genes, harbouring a total of 54 variants with predicted pathogenic effects. In 18 genes, we identified 36 compound heterozygous variants, whereas in the other 18 genes we identified 18 de novo variants. Twelve of 36 candidate risk genes are known to play a role in transmembrane transport, adaptive and innate immunity, and epithelial barrier function. CONCLUSIONS The 36 candidate genes for early‐onset PSC need further verification in other patient cohorts and evaluation of gene function before a causal role can be attributed to its variants.
AbstractList	BACKGROUND & AIMS Primary sclerosing cholangitis (PSC) is a rare bile duct disease strongly associated with inflammatory bowel disease (IBD). Whole‐exome sequencing (WES) has contributed to understanding the molecular basis of very early‐onset IBD, but rare protein‐altering genetic variants have not been identified for early‐onset PSC. We performed WES in patients diagnosed with PSC ≤ 12 years to investigate the contribution of rare genetic variants to early‐onset PSC. METHODS In this multicentre study, WES was performed on 87 DNA samples from 29 patient‐parent trios with early‐onset PSC. We selected rare (minor allele frequency < 2%) coding and splice‐site variants that matched recessive (homozygous and compound heterozygous variants) and dominant (de novo) inheritance in the index patients. Variant pathogenicity was predicted by an in‐house developed algorithm (GAVIN), and PSC‐relevant variants were selected using gene expression data and gene function. RESULTS In 22 of 29 trios we identified at least 1 possibly pathogenic variant. We prioritized 36 genes, harbouring a total of 54 variants with predicted pathogenic effects. In 18 genes, we identified 36 compound heterozygous variants, whereas in the other 18 genes we identified 18 de novo variants. Twelve of 36 candidate risk genes are known to play a role in transmembrane transport, adaptive and innate immunity, and epithelial barrier function. CONCLUSIONS The 36 candidate genes for early‐onset PSC need further verification in other patient cohorts and evaluation of gene function before a causal role can be attributed to its variants. Primary sclerosing cholangitis (PSC) is a rare bile duct disease strongly associated with inflammatory bowel disease (IBD). Whole-exome sequencing (WES) has contributed to understanding the molecular basis of very early-onset IBD, but rare protein-altering genetic variants have not been identified for early-onset PSC. We performed WES in patients diagnosed with PSC ≤ 12 years to investigate the contribution of rare genetic variants to early-onset PSC. In this multicentre study, WES was performed on 87 DNA samples from 29 patient-parent trios with early-onset PSC. We selected rare (minor allele frequency < 2%) coding and splice-site variants that matched recessive (homozygous and compound heterozygous variants) and dominant (de novo) inheritance in the index patients. Variant pathogenicity was predicted by an in-house developed algorithm (GAVIN), and PSC-relevant variants were selected using gene expression data and gene function. In 22 of 29 trios we identified at least 1 possibly pathogenic variant. We prioritized 36 genes, harbouring a total of 54 variants with predicted pathogenic effects. In 18 genes, we identified 36 compound heterozygous variants, whereas in the other 18 genes we identified 18 de novo variants. Twelve of 36 candidate risk genes are known to play a role in transmembrane transport, adaptive and innate immunity, and epithelial barrier function. The 36 candidate genes for early-onset PSC need further verification in other patient cohorts and evaluation of gene function before a causal role can be attributed to its variants. Abstract BACKGROUND & AIMS Primary sclerosing cholangitis (PSC) is a rare bile duct disease strongly associated with inflammatory bowel disease (IBD). Whole‐exome sequencing (WES) has contributed to understanding the molecular basis of very early‐onset IBD, but rare protein‐altering genetic variants have not been identified for early‐onset PSC. We performed WES in patients diagnosed with PSC ≤ 12 years to investigate the contribution of rare genetic variants to early‐onset PSC. METHODS In this multicentre study, WES was performed on 87 DNA samples from 29 patient‐parent trios with early‐onset PSC. We selected rare (minor allele frequency < 2%) coding and splice‐site variants that matched recessive (homozygous and compound heterozygous variants) and dominant (de novo) inheritance in the index patients. Variant pathogenicity was predicted by an in‐house developed algorithm (GAVIN), and PSC‐relevant variants were selected using gene expression data and gene function. RESULTS In 22 of 29 trios we identified at least 1 possibly pathogenic variant. We prioritized 36 genes, harbouring a total of 54 variants with predicted pathogenic effects. In 18 genes, we identified 36 compound heterozygous variants, whereas in the other 18 genes we identified 18 de novo variants. Twelve of 36 candidate risk genes are known to play a role in transmembrane transport, adaptive and innate immunity, and epithelial barrier function. CONCLUSIONS The 36 candidate genes for early‐onset PSC need further verification in other patient cohorts and evaluation of gene function before a causal role can be attributed to its variants. BACKGROUND & AIMSPrimary sclerosing cholangitis (PSC) is a rare bile duct disease strongly associated with inflammatory bowel disease (IBD). Whole-exome sequencing (WES) has contributed to understanding the molecular basis of very early-onset IBD, but rare protein-altering genetic variants have not been identified for early-onset PSC. We performed WES in patients diagnosed with PSC ≤ 12 years to investigate the contribution of rare genetic variants to early-onset PSC. METHODSIn this multicentre study, WES was performed on 87 DNA samples from 29 patient-parent trios with early-onset PSC. We selected rare (minor allele frequency < 2%) coding and splice-site variants that matched recessive (homozygous and compound heterozygous variants) and dominant (de novo) inheritance in the index patients. Variant pathogenicity was predicted by an in-house developed algorithm (GAVIN), and PSC-relevant variants were selected using gene expression data and gene function. RESULTSIn 22 of 29 trios we identified at least 1 possibly pathogenic variant. We prioritized 36 genes, harbouring a total of 54 variants with predicted pathogenic effects. In 18 genes, we identified 36 compound heterozygous variants, whereas in the other 18 genes we identified 18 de novo variants. Twelve of 36 candidate risk genes are known to play a role in transmembrane transport, adaptive and innate immunity, and epithelial barrier function. CONCLUSIONSThe 36 candidate genes for early-onset PSC need further verification in other patient cohorts and evaluation of gene function before a causal role can be attributed to its variants.
Author	Koot, Bart G. P. Norbruis, Obbe Rheenen, Patrick F. Wolters, Victorien Koskela, Jukka Barbieri, Ruggero Weersma, Rinse K. Daly, Mark J. Koning, Barbara A. E. Xavier, Ramnik J. Jansen, Dianne B. H. Rivas, Manuel A. Visschedijk, Marijn C. Verkade, Henkjan J. Festen, Eleonora A. M. Stevens, Christine Diemen, Cleo C. Meij, Tim Joosse, Maria E. Haisma, Sjoukje‐Marije
AuthorAffiliation	2 Department of Gastroenterology and Hepatology University of Groningen University Medical Center Groningen Groningen The Netherlands 6 Department of Pediatric Gastroenterology University Medical Center Utrecht – Wilhelmina Children's Hospital Utrecht The Netherlands 13 Department of Genetics University of Groningen University Medical Center Groningen Groningen The Netherlands 1 Department of Paediatric Gastroenterology Hepatology and Nutrition University of Groningen University Medical Center Groningen Groningen The Netherlands 12 Stanford University Stanford CA United States 3 Department of Paediatric Gastroenterology Erasmus University Medical Center Sophia Children's Hospital Rotterdam The Netherlands 9 Massachusetts General Hospital, Gastroenterology Boston MA USA 8 Broad Institute of Harvard and Massachusetts Institute of Technology Boston MA USA 11 Clinic of Gastroenterology Helsinki Helsinki University and Helsinki University Hospital Helsinki Finland 7 Department of Pediatrics Isala Ho
AuthorAffiliation_xml	– name: 11 Clinic of Gastroenterology Helsinki Helsinki University and Helsinki University Hospital Helsinki Finland – name: 1 Department of Paediatric Gastroenterology Hepatology and Nutrition University of Groningen University Medical Center Groningen Groningen The Netherlands – name: 10 Institute for Molecular Medicine Finland (FIMM) University of Helsinki Helsinki Finland – name: 5 Pediatric Gastroenterology Emma Children's Hospital Amsterdam UMC University of Amsterdam Amsterdam The Netherlands – name: 3 Department of Paediatric Gastroenterology Erasmus University Medical Center Sophia Children's Hospital Rotterdam The Netherlands – name: 8 Broad Institute of Harvard and Massachusetts Institute of Technology Boston MA USA – name: 4 Department of Pediatric Gastroenterology VU University Medical Center Amsterdam The Netherlands – name: 2 Department of Gastroenterology and Hepatology University of Groningen University Medical Center Groningen Groningen The Netherlands – name: 9 Massachusetts General Hospital, Gastroenterology Boston MA USA – name: 7 Department of Pediatrics Isala Hospital Zwolle The Netherlands – name: 12 Stanford University Stanford CA United States – name: 6 Department of Pediatric Gastroenterology University Medical Center Utrecht – Wilhelmina Children's Hospital Utrecht The Netherlands – name: 13 Department of Genetics University of Groningen University Medical Center Groningen Groningen The Netherlands
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Copyright	2021 The Authors. published by John Wiley & Sons Ltd. 2021 The Authors. Liver International published by John Wiley & Sons Ltd. 2021. This article is published under http://creativecommons.org/licenses/by-nc/4.0/ (the “License”). Notwithstanding the ProQuest Terms and Conditions, you may use this content in accordance with the terms of the License.
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Notes	FUNDING INFORMATION This work was supported by the European Crohn's and Colitis Organization (ECCO) [grant number Grant_2017/ECCO/PatrickvanRheenen]. ObjectType-Article-1 SourceType-Scholarly Journals-1 ObjectType-Feature-2 content type line 23 Patrick F van Rheenen, Cleo C van Diemen are shared last authors. Handling Editor: Ana Lleo
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Snippet	BACKGROUND & AIMS Primary sclerosing cholangitis (PSC) is a rare bile duct disease strongly associated with inflammatory bowel disease (IBD). Whole‐exome... Primary sclerosing cholangitis (PSC) is a rare bile duct disease strongly associated with inflammatory bowel disease (IBD). Whole-exome sequencing (WES) has... Abstract BACKGROUND & AIMS Primary sclerosing cholangitis (PSC) is a rare bile duct disease strongly associated with inflammatory bowel disease (IBD).... BACKGROUND & AIMSPrimary sclerosing cholangitis (PSC) is a rare bile duct disease strongly associated with inflammatory bowel disease (IBD). Whole‐exome... BACKGROUND & AIMSPrimary sclerosing cholangitis (PSC) is a rare bile duct disease strongly associated with inflammatory bowel disease (IBD). Whole-exome...
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SubjectTerms	Algorithms Bile ducts Cholangitis Deoxyribonucleic acid DNA Gene expression Gene frequency Genes genetic Genetic diversity Genetic variance Genetics and Rare Liver Diseases Heredity Inflammatory bowel disease Inflammatory bowel diseases Innate immunity Intestine Original Pathogenicity Pathogens sclerosing cholangitis
Title	Exome sequencing in patient‐parent trios suggests new candidate genes for early‐onset primary sclerosing cholangitis
URI	https://onlinelibrary.wiley.com/doi/abs/10.1111%2Fliv.14831 https://www.ncbi.nlm.nih.gov/pubmed/33590606 https://www.proquest.com/docview/2513339307 https://search.proquest.com/docview/2490131187 https://pubmed.ncbi.nlm.nih.gov/PMC8252477
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