Abstract

Hirschsprung disease (HRSD), or aganglionic megacolon, is a disorder associated with the lack of intrinsic ganglion cells in the myentric and submucosal plexuses in the gastrointestinal tract. Clinically, the phenotype may be mild, intermediate or severe. The incidence of severe HRSD is 1/5,000 livebirths, and males are more likely to be affected than females. The etiologies of this developmental disorder are unknown, but failure of neural crest cells or preenteric/enteric ganglion cells to migrate, differentiate or colonize the gut could result in HRSD. The postulated defects are in cell-cell or cell-substrate adhesion of ganglion cells. It is assumed that HRSD is a sex-modified multifactorial disorder. Our recent studies, however, demonstrate dominant inheritance for long segment HRSD (aganglionosis of the transverse colon and beyond), dominant inheritance for short segment HRSD (aganglionosis of the splenic flexure and descending colon) and multifactorial/recessive inheritance for the """"""""classic"""""""" type HRSD (aganglionosis up to and including the sigmoid colon). The penetrances of these genes are incomplete. To identify genetic factors leading to HRSD three studies are proposed. First, we shall perform high resolution prophase banding and cytogenetic analysis on 20 probands with multiple anomalies to identify consistent chromosomal aberrations. Second, we shall use highly polymorphic DNA probes to search for microdeletions within chromosome 13q22 in 50 simplex families. Third, we shall study highly polymorphic DNA markers and perform linkage in a minimum of 6 large pedigrees and in 60 affected sib and other relative pairs, to identify regions of the human genome that contain genes predisposing to HRSD. The genetic markers to be used will be selected on the basis of three criteria: localizations of known chromosomal aberrations; candidate genes responsible for cell-cell and cell-substrate adhesion; and, human chromosomal segments homologous to mouse chromosomal segments containing mutations causing aganglionosis in the mouse. Specifically, our aim is to identify genetic etiologies of HRSD and study the effects of abnormalities of cell adhesion on human pathology. Also, we aim to elucidate the relationship between the genes identified, extent of aganglionosis and severity of symptoms. Generally, our studies have the long-term objective of providing a logical approach to identifying the genes predisposing to complex, """"""""multifactorial"""""""" disorders.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
Eunice Kennedy Shriver National Institute of Child Health & Human Development (NICHD)
Type
Research Project (R01)
Project #
5R01HD028088-03
Application #
3329709
Study Section
Mammalian Genetics Study Section (MGN)
Project Start
1991-04-01
Project End
1994-03-31
Budget Start
1993-04-01
Budget End
1994-03-31
Support Year
3
Fiscal Year
1993
Total Cost
Indirect Cost

  Institution

Name
University of Pittsburgh
Department
Type
Schools of Public Health
DUNS #
053785812
City
Pittsburgh
State
PA
Country
United States
Zip Code
15213

  Publications

Fadista, João; Lund, Marie; Skotte, Line et al. (2018) Genome-wide association study of Hirschsprung disease detects a novel low-frequency variant at the RET locus. Eur J Hum Genet 26:561-569
Kapoor, Ashish; Auer, Dallas R; Lee, Dongwon et al. (2017) Testing the Ret and Sema3d genetic interaction in mouse enteric nervous system development. Hum Mol Genet 26:1811-1820
Chatterjee, Sumantra; Kapoor, Ashish; Akiyama, Jennifer A et al. (2016) Enhancer Variants Synergistically Drive Dysfunction of a Gene Regulatory Network In Hirschsprung Disease. Cell 167:355-368.e10
Tang, Clara Sze-Man; Gui, Hongsheng; Kapoor, Ashish et al. (2016) Trans-ethnic meta-analysis of genome-wide association studies for Hirschsprung disease. Hum Mol Genet 25:5265-5275
Khayat, Morad; Tilghman, Joseph Mark; Chervinsky, Ilana et al. (2016) A PIGN mutation responsible for multiple congenital anomalies-hypotonia-seizures syndrome 1 (MCAHS1) in an Israeli-Arab family. Am J Med Genet A 170A:176-82
Kapoor, Ashish; Jiang, Qian; Chatterjee, Sumantra et al. (2015) Population variation in total genetic risk of Hirschsprung disease from common RET, SEMA3 and NRG1 susceptibility polymorphisms. Hum Mol Genet 24:2997-3003
Jiang, Qian; Arnold, Stacey; Heanue, Tiffany et al. (2015) Functional loss of semaphorin 3C and/or semaphorin 3D and their epistatic interaction with ret are critical to Hirschsprung disease liability. Am J Hum Genet 96:581-96
Gunadi; Kapoor, Ashish; Ling, Albee Yun et al. (2014) Effects of RET and NRG1 polymorphisms in Indonesian patients with Hirschsprung disease. J Pediatr Surg 49:1614-8
Jiang, Qian; Turner, Tychele; Sosa, Maria X et al. (2012) Rapid and efficient human mutation detection using a bench-top next-generation DNA sequencer. Hum Mutat 33:281-9
Emison, Eileen Sproat; Garcia-Barcelo, Merce; Grice, Elizabeth A et al. (2010) Differential contributions of rare and common, coding and noncoding Ret mutations to multifactorial Hirschsprung disease liability. Am J Hum Genet 87:60-74

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