Abstract
Xenopus embryos are covered with a complex epithelium containing numerous multiciliated cells (MCCs). During late-stage development, there is a dramatic remodeling of the epithelium that involves the complete loss of MCCs. Cell extrusion is awell-characterized process for driving cell loss while maintaining epithelial barrier function. Normal cell extrusion is typically unidirectional, whereas bidirectional extrusion is often associated with disease (e.g. cancer).We describe two distinct mechanisms for MCC extrusion, a basal extrusion driven by Notch signaling and an apical extrusion driven by Piezo1. Early in the process there is a strong bias towards basal extrusion, but as development continues there is a shift towards apical extrusion. Importantly, response to the Notch signal is age dependent and governed by the maintenance of the MCC transcriptional program such that extension of this program is protective against cell loss. In contrast, later apical extrusion is regulated by Piezo1, such that premature activation of Piezo1 leads to early extrusion while blocking Piezo1 leads to MCC maintenance. Distinct mechanisms for MCC loss underlie the importance of their removal during epithelial remodeling.
| Original language | English (US) |
|---|---|
| Article number | dev.201612 |
| Journal | Development (Cambridge) |
| Volume | 150 |
| Issue number | 17 |
| DOIs | |
| State | Published - Sep 2023 |
Funding
This work was supported by the National Institutes of Health (GM089970 to B.M, TGM32AR060710 to R.V. and a diversity supplement from GM119322 to O.H.). P.W. was supported by the Deutsche Forschungsgemeinschaft under the Emmy Noether Programme (WA3365/2-1) and under Germany’s Excellence Strategy (CIBSS – EXC-2189 – Project ID 390939984). Open Access funding provided by Northwestern University. Deposited in PMC for immediate release.
Keywords
- Cell extrusion
- Multiciliated cells
- Notch
- Piezo1
ASJC Scopus subject areas
- Molecular Biology
- Developmental Biology
