| Literature DB >> 30874462 |
Neylen Del Toro1, Ana Fernandez-Ruiz1,2, Lian Mignacca1, Paloma Kalegari1,2, Marie-Camille Rowell1,2, Sebastian Igelmann1, Emmanuelle Saint-Germain1, Mehdi Benfdil1, Stéphane Lopes-Paciencia1,2, Léa Brakier-Gingras1, Véronique Bourdeau1, Gerardo Ferbeyre1,2, Frédéric Lessard1.
Abstract
Senescence is a tumor suppressor program characterized by a stable growth arrest while maintaining cell viability. Senescence-associated ribogenesis defects (SARD) have been shown to regulate senescence through the ability of the ribosomal protein S14 (RPS14 or uS11) to bind and inhibit the cyclin-dependent kinase 4 (CDK4). Here we report another ribosomal protein that binds and inhibits CDK4 in senescent cells: L22 (RPL22 or eL22). Enforcing the expression of RPL22/eL22 is sufficient to induce an RB and p53-dependent cellular senescent phenotype in human fibroblasts. Mechanistically, RPL22/eL22 can interact with and inhibit CDK4-Cyclin D1 to decrease RB phosphorylation both in vitro and in cells. Briefly, we show that ribosome-free RPL22/eL22 causes a cell cycle arrest which could be relevant during situations of nucleolar stress such as cellular senescence or the response to cancer chemotherapy.Entities:
Keywords: CDK4; RPL22/eL22; RPS14/uS11; Ribosome biogenesis; cyclin D1; senescence
Year: 2019 PMID: 30874462 PMCID: PMC6464582 DOI: 10.1080/15384101.2019.1593708
Source DB: PubMed Journal: Cell Cycle ISSN: 1551-4005 Impact factor: 4.534