| Literature DB >> 33495473 |
Nao Sankoda1,2,3, Wataru Tanabe1,4, Akito Tanaka1, Hirofumi Shibata5, Knut Woltjen1,6, Tsutomu Chiba4, Hironori Haga7, Yoshiharu Sakai2, Masaki Mandai8, Takuya Yamamoto1,9,10,11, Yasuhiro Yamada3,9, Shinji Uemoto2, Yoshiya Kawaguchi12.
Abstract
The squamous-columnar junction (SCJ) is a boundary consisting of precisely positioned transitional epithelium between the squamous and columnar epithelium. Transitional epithelium is a hotspot for precancerous lesions, and is therefore clinically important; however, the origins and physiological properties of transitional epithelium have not been fully elucidated. Here, by using mouse genetics, lineage tracing, and organoid culture, we examine the development of the SCJ in the mouse stomach, and thus define the unique features of transitional epithelium. We find that two transcription factors, encoded by Sox2 and Gata4, specify primitive transitional epithelium into squamous and columnar epithelium. The proximal-distal segregation of Sox2 and Gata4 expression establishes the boundary of the unspecified transitional epithelium between committed squamous and columnar epithelium. Mechanistically, Gata4-mediated expression of the morphogen Fgf10 in the distal stomach and Sox2-mediated Fgfr2 expression in the proximal stomach induce the intermediate regional activation of MAPK/ERK, which prevents the differentiation of transitional epithelial cells within the SCJ boundary. Our results have implications for tissue regeneration and tumorigenesis, which are related to the SCJ.Entities:
Year: 2021 PMID: 33495473 PMCID: PMC7835245 DOI: 10.1038/s41467-021-20906-0
Source DB: PubMed Journal: Nat Commun ISSN: 2041-1723 Impact factor: 14.919