Abstract
AbstractEpithelial branching morphogenesis is an essential process in living organisms, through which organ-specific epithelial shapes are created. Interactions between epithelial cells and their stromal microenvironment instruct branching morphogenesis but remain incompletely understood. Here we employed fibroblast-organoid or fibroblast-spheroid co-culture systems and time-lapse imaging to reveal that physical contact between fibroblasts and epithelial cells and fibroblast contractility are required to induce mammary epithelial branching. Pharmacological inhibition of ROCK or non-muscle myosin II, or fibroblast-specific knock-out ofMyh9abrogate fibroblast-induced epithelial branching. Furthermore, fibroblast-induced branching requires epithelial proliferation and is associated with distinctive epithelial patterning of YAP and ERK activity along organoid branches, which is dependent on fibroblast contractility. Together, we identify fibroblast contractility as a novel stromal factor driving mammary epithelial morphogenesis. Our study contributes to comprehensive understanding of overlapping but divergent employment of mechanically active fibroblasts in developmental versus tumorigenic programs.
Publisher
Cold Spring Harbor Laboratory
Cited by
1 articles.
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