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Wnt/Fgf crosstalk is required for the specification of basal cells in the mouse trachea. | LitMetric

Basal progenitor cells are crucial for the establishment and maintenance of the tracheal epithelium. However, it remains unclear how these progenitor cells are specified during foregut development. Here, we found that ablation of the Wnt chaperone protein Gpr177 (also known as Wntless) in mouse tracheal epithelium causes a significant reduction in the number of basal progenitor cells accompanied by cartilage loss in mutants. Consistent with the association between cartilage and basal cell development, Nkx2.1p63 basal cells are co-present with cartilage nodules in mutants, which maintain partial cell-cell adhesion but not the transcription regulation function of β-catenin. More importantly, deletion of in the mesenchyme leads to the loss of basal cells and cartilage, concomitant with reduced transcript levels of Fgf10 in mutants. Furthermore, deletion of Fgf receptor 2 () in the epithelium also leads to significantly reduced numbers of basal cells, supporting the importance of Wnt/Fgf crosstalk in early tracheal development.

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http://www.ncbi.nlm.nih.gov/pmc/articles/PMC6382003PMC
http://dx.doi.org/10.1242/dev.171496DOI Listing

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