Litcius/Paper detail

p63 and Its Target Follistatin Maintain Salivary Gland Stem/Progenitor Cell Function through TGF-β/Activin Signaling

Sangwon Min, Akinsola Oyelakin, Christian Gluck, Jonathan Bard, Eun‐Ah Christine Song, Kirsten Smalley, Monika Che, Elsa R. Flores, Satrajit Sinha, Rose‐Anne Romano

2020iScience29 citationsDOIOpen Access PDF

Abstract

Multipotent ΔNp63-positive cells maintain all epithelial cell lineages of the embryonic and adult salivary gland (SG). However, the molecular mechanisms by which ΔNp63 regulates stem/progenitor (SP) cell populations in the SG remains elusive. To understand the role of ΔNp63 in directing cell fate choices in this gland, we have generated ΔNp63-deleted adult mice and primary salivary cell cultures to probe alterations in SP cell differentiation and function. In parallel, we have leveraged RNA-seq and ChIP-seq-based characterization of the ΔNp63-driven cistrome and scRNA-seq analysis to molecularly interrogate altered SG cellular identities and differentiation states dependent on ΔNp63. Our studies reveal that ablation of ΔNp63 results in a loss of the SP cell population and skewed differentiation that is mediated by Follistatin-dependent dysregulated TGF-β/Activin signaling. These findings offer new revelations into the SP cell gene regulatory networks that are likely to be relevant for normal or diseased SG states.

Topics & Concepts

FollistatinProgenitor cellBiologyCell biologyEmbryonic stem cellStem cellCellular differentiationPopulationProgenitorCellCell fate determinationTranscription factorGeneticsGeneMedicineEnvironmental healthdental development and anomaliesTGF-β signaling in diseasesSalivary Gland Tumors Diagnosis and Treatment