Genome-wide association study identifies
            <i>NRG1</i>
            as a susceptibility locus for Hirschsprung's disease

García-Barceló, María-Mercé; Tang, Clara S.; Ngan, Elly Sau-Wai; Lui, Vincent Chi-Hang; Chen, Yan; So, Man-Ting; Leon, Thomas Y.Y.; Miao, Xiaoping; Shum, Cathy K.Y.; Liu, Fengqin; Yeung, Ming-Yiu; Yuan, Zhenwei; Guo, Weihong; Liu, Lei; Sun, Xiao-bing; Huang, Liuming; Tou, Jinfa; Song, You‐Qiang; Chan, Danny; Cheung, Kenneth M.C.; Wong, Kenneth K.; Cherny, Stacey S.; Sham, Pak-Chung; Tam, Paul Kwong‐Hang

doi:10.1073/pnas.0809630105

Cited by 171 publications

(202 citation statements)

References 48 publications

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“…Other UC-specific regions are found at chromosome 1p36 and 12q15 [12] , however, at these loci, the exact disease genes remain to be identified. The association of classical HLA alleles and UC is well known [63] , and also (20q13) [202] Colorectal [120] If the authors mainly reported one region with several candidate genes the region is listed with the candidates in the region in parentheses, while if a specific gene was reported this is listed. Where more than one panel was used, but jointly analyzed, the sum of cases and controls in these panels is listed.…”

Section: Bowel Diseases (See Table 2 For Details)mentioning

confidence: 99%

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Genome-wide association studies - A summary for theclinical gastroenterologist

Melum¹,

Franke²,

Karlsen³

2009

WJG

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Genome-wide association studies (GWAS) have been applied to various gastrointestinal and liver diseases in recent years. A large number of susceptibility genes and key biological pathways in disease development have been identified. So far, studies in inflammatory bowel diseases, and in particular Crohn's disease, have been especially successful in defining new susceptibility loci using the GWAS design. The identification of associations related to autophagy as well as several genes involved in immunological response will be important to future research on Crohn's disease. In this review, key methodological aspects of GWAS, the importance of proper cohort collection, genotyping issues and statistical methods are summarized. Ways of addressing the shortcomings of the GWAS design, when it comes to rare variants, are also discussed. For each of the relevant conditions, findings from the various GWAS are summarized with a focus on the affected biological systems.

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Section: Bowel Diseases (See Table 2 For Details)mentioning

confidence: 99%

“…For a large proportion of familial cases and a considerable amount of sporadic cases, it has long been known that mutations in the RET gene are important [119] . In a small GWAS, Garcia-Barcelo et al [120] recently made several important discoveries. Firstly, they confirmed the associations previously detected at the RET locus.…”

Section: Celiac Diseasementioning

confidence: 99%

Genome-wide association studies - A summary for theclinical gastroenterologist

Melum¹,

Franke²,

Karlsen³

2009

WJG

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“…Yet, despite the importance of RET, additional genes (acting either in conjunction or independently from RET) are necessary to explain not only the disease incidence but also its complex pattern of inheritance. Other HSCR genes identified so far mainly code for protein members of inter-related signaling pathways involved in the ENS development: endothelin receptor B (EDNRB), the transcriptional regulator SOX10, and the NRG1/ERBB2 signaling pathway gene (Hofstra et al, 1999;Heanue & Pachnis, 2007;Garcia-Barcelo et al, 2009). CDS mutations in genes other than RET thus far only account for 7% of the cases; however, the unexplained phenotypic variance in sporadic HSCR cases is still very high (>80%) (Gui et al, 2013).…”

Section: Introductionmentioning

confidence: 99%

“…All of the 14 genes known to cause HSCR in human newborns and ENS failure in the embryonic mouse (Table 1) were compulsorily included, while the other 48 genes (Table S1) were selected according to the following reasons: (1) key members in the same signaling pathway with know HSCR genes; (2) genes with suggestive association with HSCR in our previous GWAS study (Garcia-Barcelo et al, 2009); (3) supported by murine or functional studies as outlined in Table S1.…”

Section: Gene Selectionmentioning

confidence: 99%

“…This pool was selected since all those five patients were also genotyped by Affymetrix 500K in our previous genome-wide association study (Garcia-Barcelo et al, 2009). The same RainDance technology was used to capture and enrich coding sequences of 62 candidate genes; however, DNA template was prepared using independent index primers for each individual without pooling and was then sequenced on an Illumina GAIIX platform (Illumina, San Diego, CA, USA).…”

Section: Technical Validationmentioning

confidence: 99%

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Targeted Next-Generation Sequencing on Hirschsprung Disease: A Pilot Study Exploits DNA Pooling

Gui

Bao

Tang

et al. 2014

Annals of Human Genetics

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SummaryTo adopt an efficient approach of identifying rare variants possibly related to Hirschsprung disease (HSCR), a pilot study was set up to evaluate the performance of a newly designed protocol for next generation targeted resquencing. In total, 20 Chinese HSCR patients and 20 Chinese sex-matched individuals with no HSCR were included, for which coding sequences (CDS) of 62 genes known to be in signaling pathways relevant to enteric nervous system development were selected for capture and sequencing. Blood DNAs from eight pools of five cases or controls were enriched by PCR-based RainDance technology (RDT) and then sequenced on a 454 FLX platform. As technical validation, five patients from case Pool-3 were also independently enriched by RDT, indexed with barcode and sequenced with sufficient coverage. Assessment for CDS single nucleotide variants showed DNA pooling performed well (specificity/sensitivity at 98.4%/83.7%) at the common variant level; but relatively worse (specificity/sensitivity at 65.5%/61.3%) at the rare variant level. Further Sanger sequencing only validated five out of 12 rare damaging variants likely involved in HSCR. Hence more improvement at variant detection and sequencing technology is needed to realize the potential of DNA pooling for large-scale resequencing projects.

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Phenotypic spectrum associated with pathogenic mutation in the NRG1 gene in Acadian family

Bourcier

Crapoulet

Ouellette

et al. 2021

American J of Med Genetics Pt A

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NRG1 is a gene that encodes for a protein that binds to a receptor of the tyrosine kinase family which is essential for the survival of the central nervous system development during embryogenesis. Mutation of the NRG1 gene causes aganglionosis, which leads to Hirschsprung disease. Two brothers of Acadian descent presented with a history of Hirschsprung disease, in association with other anomalies including congenital heart disease, learning difficulties, developmental issues, and hypopigmented hair patch. Molecular analysis in both siblings revealed a heterozygous pathogenic mutation in the NGR1 gene (c.235C>T [p.Arg79*]), that was inherited from an unaffected father. This family expands our knowledge about the phenotypic spectrum associated with pathogenic mutation in the NRG1 gene with intrafamilial variability and the likely reduced penetrance for the phenotypic expression.

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Genome-wide association study identifies NRG1 as a susceptibility locus for Hirschsprung's disease

Cited by 171 publications

References 48 publications

Genome-wide association studies - A summary for theclinical gastroenterologist

Genome-wide association studies - A summary for theclinical gastroenterologist

Targeted Next-Generation Sequencing on Hirschsprung Disease: A Pilot Study Exploits DNA Pooling

Phenotypic spectrum associated with pathogenic mutation in the NRG1 gene in Acadian family

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