Article ID Journal Published Year Pages File Type
2040245 Cell Reports 2014 11 Pages PDF
Abstract

•3D esophageal organoids generated in vitro reflect in vivo tissue architecture•Cell-surface markers separate subpopulations of mouse esophageal basal epithelium•Subpopulations have distinct differentiation and proliferation properties•A nonquiescent stem cell population resides in the basal layer of the esophagus

SummaryBecause the esophageal epithelium lacks a defined stem cell niche, it is unclear whether all basal epithelial cells in the adult esophagus are functionally equivalent. In this study, we showed that basal cells in the mouse esophagus contained a heterogeneous population of epithelial cells, similar to other rapidly cycling tissues such as the intestine or skin. Using a combination of cell-surface markers, we separated primary esophageal tissue into distinct cell populations that harbored differences in stem cell potential. We also used an in vitro 3D organoid assay to demonstrate that Sox2, Wnt, and bone morphogenetic protein signaling regulate esophageal self-renewal. Finally, we labeled proliferating basal epithelial cells in vivo to show differing cell-cycle profiles and proliferation kinetics. Based on our results, we propose that a nonquiescent stem cell population resides in the basal epithelium of the mouse esophagus.

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