Hedgehog/Notch-induced premature gliogenesis represents a new disease mechanism for Hirschsprung disease in mice and humans
Elly Sau-Wai Ngan, … , Vincent Chi-Hang Lui, Paul Kwong-Hang Tam
Elly Sau-Wai Ngan, … , Vincent Chi-Hang Lui, Paul Kwong-Hang Tam
Published August 15, 2011
Citation Information: J Clin Invest. 2011;121(9):3467-3478. https://doi.org/10.1172/JCI43737.
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Research Article Gastroenterology

Hedgehog/Notch-induced premature gliogenesis represents a new disease mechanism for Hirschsprung disease in mice and humans

Abstract

Hirschsprung (HSCR) disease is a complex genetic disorder attributed to a failure of the enteric neural crest cells (ENCCs) to form ganglia in the hindgut. Hedgehog and Notch are implicated in mediating proliferation and differentiation of ENCCs. Nevertheless, how these signaling molecules may interact to mediate gut colonization by ENCCs and contribute to a primary etiology for HSCR are not known. Here, we report our pathway-based epistasis analysis of data generated by a genome-wide association study on HSCR disease, which indicates that specific genotype constellations of Patched (PTCH1) (which encodes a receptor for Hedgehog) and delta-like 3 (DLL3) (which encodes a receptor for Notch) SNPs confer higher risk to HSCR. Importantly, deletion of Ptch1 in mouse ENCCs induced robust Dll1 expression and activation of the Notch pathway, leading to premature gliogenesis and reduction of ENCC progenitors in mutant bowels. Dll1 integrated Hedgehog and Notch pathways to coordinate neuronal and glial cell differentiation during enteric nervous system development. In addition, Hedgehog-mediated gliogenesis was found to be highly conserved, such that Hedgehog was consistently able to promote gliogenesis of human neural crest–related precursors. Collectively, we defined PTCH1 and DLL3 as HSCR susceptibility genes and suggest that Hedgehog/Notch-induced premature gliogenesis may represent a new disease mechanism for HSCR.

Authors

Elly Sau-Wai Ngan, Maria-Mercè Garcia-Barceló, Benjamin Hon-Kei Yip, Hiu-Ching Poon, Sin-Ting Lau, Carmen Ka-Man Kwok, Eric Sat, Mai-Har Sham, Kenneth Kak-Yuen Wong, Brandon J. Wainwright, Stacey S. Cherny, Chi-Chung Hui, Pak Chung Sham, Vincent Chi-Hang Lui, Paul Kwong-Hang Tam

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Figure 7

Hh induces gliogenesis of SKPs.

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Hh induces gliogenesis of SKPs. (A) SKPs isolated from human foreskin co...
(A) SKPs isolated from human foreskin could give rise to cells expressing neuronal and glial markers. SKP spheres were obtained 2 to 3 weeks after culture. Immunocytochemistry showed that SKPs express precursor marker (vimentin, green). Two weeks after culturing in the differentiation medium, cells expressing neuronal (neurofilament [NFM+], red) and glial (GFAP, red) markers were observed. Cells were counterstained with DAPI (blue). Scale bar: 50 μm. (B) The percentages of glial (GFAP+) cells in untreated control and Shh-treated culture were counted over total number of cells (DAPI). Error bars indicated ± SEM of triplicates. Data was analyzed by t test. P values of less than 0.05 were considered to be statistically significant.