| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 5658423 | Gastroenterology | 2017 | 70 Pages |
Abstract
We identified mutations in VCL associated with S-HSCR. Correction of this mutation in iPSC using CRISPR/Cas9 editing, as well as the RET G731del mutation that causes Hirschsprung disease with total colonic aganglionosis, restored ENCC function. Our study demonstrates how human iPSCs can be used to identify disease-associated mutations and determine how they affect cell functions and contribute to pathogenesis.
Keywords
GDNFENCChiPSCNCDCRISPRNCMPTCAgRNAclustered regularly interspaced short palindromic repeatsNeural developmentCNSguide RNARetinoic acidCodingHuman induced pluripotent stem cellenteric nervous systemcentral nervous systemNoncodingglial cell-derived neurotrophic factorCongenitalwild-typeFocal adhesionTotal colonic aganglionosis
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Authors
Frank Pui-Ling Lai, Sin-Ting Lau, John Kwong-Leong Wong, Hongsheng Gui, Reeson Xu Wang, Tingwen Zhou, Wing Hon Lai, Hung-Fat Tse, Paul Kwong-Hang Tam, Maria-Mercedes Garcia-Barcelo, Elly Sau-Wai Ngan,