Biology Open (Feb 2015)

Transforming Growth Factor β/activin signalling induces epithelial cell flattening during Drosophila oogenesis

  • Isabelle Brigaud,
  • Jean-Luc Duteyrat,
  • Julien Chlasta,
  • Sandrine Le Bail,
  • Jean-Louis Couderc,
  • Muriel Grammont

DOI
https://doi.org/10.1242/bio.201410785
Journal volume & issue
Vol. 4, no. 3
pp. 345 – 354

Abstract

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Although the regulation of epithelial morphogenesis is essential for the formation of tissues and organs in multicellular organisms, little is known about how signalling pathways control cell shape changes in space and time. In the Drosophila ovarian epithelium, the transition from a cuboidal to a squamous shape is accompanied by a wave of cell flattening and by the ordered remodelling of E-cadherin-based adherens junctions. We show that activation of the TGFβ pathway is crucial to determine the timing, the degree and the dynamic of cell flattening. Within these cells, TGFβ signalling controls cell-autonomously the formation of Actin filament and the localisation of activated Myosin II, indicating that internal forces are generated and used to remodel AJ and to promote cytoskeleton rearrangement. Our results also reveal that TGFβ signalling controls Notch activity and that its functions are partly executed through Notch. Thus, we demonstrate that the cells that undergo the cuboidal-to-squamous transition produce active cell-shaping mechanisms, rather than passively flattening in response to a global force generated by the growth of the underlying cells. Thus, our work on TGFβ signalling provides new insights into the mechanisms through which signal transduction cascades orchestrate cell shape changes to generate proper organ structure.

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