2015
DOI: 10.1016/j.ajhg.2015.02.014
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Functional Loss of Semaphorin 3C and/or Semaphorin 3D and Their Epistatic Interaction with Ret Are Critical to Hirschsprung Disease Liability

Abstract: Innervation of the gut is segmentally lost in Hirschsprung disease (HSCR), a consequence of cell-autonomous and non-autonomous defects in enteric neuronal cell differentiation, proliferation, migration, or survival. Rare, high-penetrance coding variants and common, low-penetrance non-coding variants in 13 genes are known to underlie HSCR risk, with the most frequent variants in the ret proto-oncogene (RET). We used a genome-wide association (220 trios) and replication (429 trios) study to reveal a second non-c… Show more

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Cited by 122 publications
(165 citation statements)
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References 55 publications
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“…Most of the other genes have been identified in rare (familial) syndromic HSCR cases (Amiel et al, 2008). In addition to the rare, coding mutations with large effects, common, non-coding variants with small effects have also been identified (Emison et al, 2010; Jiang et al, 2015). …”
Section: What Are the Target Diseases For Stem Cell Transplantation?mentioning
confidence: 99%
“…Most of the other genes have been identified in rare (familial) syndromic HSCR cases (Amiel et al, 2008). In addition to the rare, coding mutations with large effects, common, non-coding variants with small effects have also been identified (Emison et al, 2010; Jiang et al, 2015). …”
Section: What Are the Target Diseases For Stem Cell Transplantation?mentioning
confidence: 99%
“…The best example to date lies in the additional susceptibility gene for semaphorin 3A, which results in signaling pathway dysfunction in conjunction with a variant in Ret, leading to malfunction and disease. 20 It is probable that this could function as a viable hypothesis for other identified genetic variations, in keeping with the current concept of a multigenetic etiology for HSCR. Some then lead to syndromic phenotypic expressions of genes identified in associated syndromes (eg, chromosome 21 and ZEB2 genetic variations associated with the Mowat-Wilson syndrome).…”
mentioning
confidence: 92%
“…[18][19][20] The reason for the incomplete migration and development of ganglion cells is as yet not fully understood. Early estimates were that genetic variations could be identified in at least 12% of HSCR cases, which is higher than the expected in the normal population.…”
Section: Genetic Associations Of Hscrmentioning
confidence: 99%
See 1 more Smart Citation
“…The 3 common polymorphisms were identified in genome-wide association study of HSCR patients of European ancestry and replicated independently [35, 36] The prevalence of each of the variables listed was compared between patients with and without proximal IND-SH using Welch Two Sample T-test, Fisher’s Exact test, or Permutation Chi-Squared test.…”
Section: Methodsmentioning
confidence: 99%