Notch and Prospero Repress Proliferation following Cyclin E Overexpression in the Drosophila Bristle Lineage

Understanding the mechanisms that coordinate cell proliferation, cell cycle arrest, and cell differentiation is essential to address the problem of how “normal” versus pathological developmental processes take place. In the bristle lineage of the adult fly, we have tested the capacity of post-mitotic cells to re-enter the cell cycle in response to the overexpression of cyclin E. We show that only terminal cells in which the identity is independent of Notch pathway undergo extra divisions after CycE overexpression. Our analysis shows that the responsiveness of cells to forced proliferation depends on both Prospero, a fate determinant, and on the level of Notch pathway activity. Our results demonstrate that the terminal quiescent state and differentiation are regulated by two parallel mechanisms acting simultaneously on fate acquisition and cell cycle progression.

Despite substantial progress that has been made, we still know little about how single precursor cells undergo a limited number of cell divisions before arrest. Discovering the mechanisms by which terminal cells maintain cell division arrest is essential for understanding “normal” development, as well as the origin of pathological deregulations. Using the bristle cell lineage, a model system widely employed to analye cell identity acquisition, we observed that only two out of four terminal cells in this lineage are unable to re-enter the cell cycle and proliferate. Our study shows that in these cells, cell division arrest is maintained by the action of the transcription factor Prospero and the signalling pathway Notch. Since both of these factors also control cell identity in this lineage, this finding demonstrates that common elements acting simultaneously and in parallel regulate the terminal quiescent state and differentiation. This system provides a unique animal model in which to understand how the mechanisms involved in cell fate acquisition and those controlling cell division intermingle to produce cell lineages resulting in terminal cells in the right number and at the right place and time.