Upregulation of the Nr2f1-A830082K12Rik gene pair in murine neural crest cells results in a complex phenotype reminiscent of Waardenburg syndrome type 4

Karl-F Bergeron; Chloé M A Nguyen; Tatiana Cardinal; Baptiste Charrier; David W Silversides; Nicolas Pilon

doi:10.1242/dmm.026773

Upregulation of the Nr2f1-A830082K12Rik gene pair in murine neural crest cells results in a complex phenotype reminiscent of Waardenburg syndrome type 4

Dis Model Mech. 2016 Nov 1;9(11):1283-1293. doi: 10.1242/dmm.026773. Epub 2016 Sep 1.

Authors

Karl-F Bergeron¹, Chloé M A Nguyen¹, Tatiana Cardinal¹, Baptiste Charrier¹, David W Silversides², Nicolas Pilon³

Affiliations

¹ Molecular Genetics of Development Laboratory, Department of Biological Sciences and BioMed Research Center, University of Quebec at Montreal (UQAM), Montreal, H2X 3Y7, Canada.
² Veterinary Genetics Laboratory, Faculty of Veterinary Medicine, University of Montreal, St-Hyacinthe, J2S 7C6, Canada.
³ Molecular Genetics of Development Laboratory, Department of Biological Sciences and BioMed Research Center, University of Quebec at Montreal (UQAM), Montreal, H2X 3Y7, Canada pilon.nicolas@uqam.ca.

Abstract

Waardenburg syndrome is a neurocristopathy characterized by a combination of skin and hair depigmentation, and inner ear defects. In the type 4 form, these defects show comorbidity with Hirschsprung disease, a disorder marked by an absence of neural ganglia in the distal colon, triggering functional intestinal obstruction. Here, we report that the Spot mouse line - obtained through an insertional mutagenesis screen for genes involved in neural crest cell (NCC) development - is a model for Waardenburg syndrome type 4. We found that the Spot insertional mutation causes overexpression of an overlapping gene pair composed of the transcription-factor-encoding Nr2f1 and the antisense long non-coding RNA A830082K12Rik in NCCs through a mechanism involving relief of repression of these genes. Consistent with the previously described role of Nr2f1 in promoting gliogenesis in the central nervous system, we further found that NCC-derived progenitors of the enteric nervous system fail to fully colonize Spot embryonic guts owing to their premature differentiation in glial cells. Taken together, our data thus identify silencer elements of the Nr2f1-A830082K12Rik gene pair as new candidate loci for Waardenburg syndrome type 4.

Keywords: Enteric nervous system; Hirschsprung disease; Melanocytes; Mouse model; Neural crest cells; Waardenburg syndrome.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Animals
Animals, Newborn
Base Sequence
COUP Transcription Factor I / metabolism*
Cell Differentiation / genetics
Endolymph / metabolism
Enteric Nervous System / pathology
Hirschsprung Disease / genetics*
Melanocytes / metabolism
Melanocytes / pathology
Mice
Mice, Mutant Strains
Mutagenesis, Insertional
Neural Crest / metabolism*
Neural Crest / pathology*
Neuroglia / metabolism
Neuroglia / pathology
Phenotype
Pigmentation / genetics
RNA, Long Noncoding / genetics
RNA, Long Noncoding / metabolism*
Transgenes
Up-Regulation / genetics*
Waardenburg Syndrome / genetics*

Substances

A830082K12Rik non-coding RNA, mouse
COUP Transcription Factor I
Nr2f1 protein, mouse
RNA, Long Noncoding

Supplementary concepts

Waardenburg syndrome, type 4

Grants and funding

MOP-26037/CIHR/Canada