Literature DB >> 32439755

Pitx2-Sox2-Lef1 interactions specify progenitor oral/dental epithelial cell signaling centers.

Wenjie Yu1, Zhao Sun1,2, Yan Sweat1, Mason Sweat1, Shankar Rengasamy Venugopalan3, Steven Eliason1, Huojun Cao3, Michael L Paine4, Brad A Amendt5,3.   

Abstract

Epithelial signaling centers control epithelial invagination and organ development, but how these centers are specified remains unclear. We report that Pitx2 (the first transcriptional marker for tooth development) controls the embryonic formation and patterning of epithelial signaling centers during incisor development. We demonstrate using Krt14Cre /Pitx2flox/flox (Pitx2cKO ) and Rosa26CreERT/Pitx2flox/flox mice that loss of Pitx2 delays epithelial invagination, and decreases progenitor cell proliferation and dental epithelium cell differentiation. Developmentally, Pitx2 regulates formation of the Sox2+ labial cervical loop (LaCL) stem cell niche in concert with two signaling centers: the initiation knot and enamel knot. The loss of Pitx2 disrupted the patterning of these two signaling centers, resulting in tooth arrest at E14.5. Mechanistically, Pitx2 transcriptional activity and DNA binding is inhibited by Sox2, and this interaction controls gene expression in specific Sox2 and Pitx2 co-expression progenitor cell domains. We demonstrate new transcriptional mechanisms regulating signaling centers by Pitx2, Sox2, Lef1 and Irx1.
© 2020. Published by The Company of Biologists Ltd.

Entities:  

Keywords:  Craniofacial/tooth development; Dental epithelial stem cells; Enamel knot; Irx1; Pitx2; Shh; Signaling centers; Sox2; Stem cell niche; Transcriptional regulation

Mesh:

Substances:

Year:  2020        PMID: 32439755      PMCID: PMC7286298          DOI: 10.1242/dev.186023

Source DB:  PubMed          Journal:  Development        ISSN: 0950-1991            Impact factor:   6.868


  53 in total

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