| Literature DB >> 31983631 |
Valentina C Sladky1, Katja Knapp1, Claudia Soratroi1, Julia Heppke1, Felix Eichin1, Lourdes Rocamora-Reverte1, Tamas G Szabo1, Laura Bongiovanni2, Bart Westendorp2, Eva Moreno2, Elsbeth A van Liere2, Bjorn Bakker3, Diana C J Spierings3, René Wardenaar3, David Pereyra4, Patrick Starlinger4, Simon Schultze5, Michael Trauner5, Tatjana Stojakovic6, Hubert Scharnagl6, Luca L Fava7, Floris Foijer3, Alain de Bruin8, Andreas Villunger9.
Abstract
E2F transcription factors control the cytokinesis machinery and thereby ploidy in hepatocytes. If or how these proteins limit proliferation of polyploid cells with extra centrosomes remains unknown. Here, we show that the PIDDosome, a signaling platform essential for caspase-2-activation, limits hepatocyte ploidy and is instructed by the E2F network to control p53 in the developing as well as regenerating liver. Casp2 and Pidd1 act as direct transcriptional targets of E2F1 and its antagonists, E2F7 and E2F8, that together co-regulate PIDDosome expression during juvenile liver growth and regeneration. Of note, whereas hepatocyte aneuploidy correlates with the basal ploidy state, the degree of aneuploidy itself is not limited by PIDDosome-dependent p53 activation. Finally, we provide evidence that the same signaling network is engaged to control ploidy in the human liver after resection. Our study defines the PIDDosome as a primary target to manipulate hepatocyte ploidy and proliferation rates in the regenerating liver.Entities:
Keywords: PIDDosome; caspases; liver development; p53; polyploidy; regeneration
Year: 2020 PMID: 31983631 DOI: 10.1016/j.devcel.2019.12.016
Source DB: PubMed Journal: Dev Cell ISSN: 1534-5807 Impact factor: 12.270