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- Title
P53-dependent hypusination of eIF5A affects mitochondrial translation and senescence immune surveillance.
- Authors
Jiang, Xiangli; Baig, Ali Hyder; Palazzo, Giuliana; Del Pizzo, Rossella; Bortecen, Toman; Groessl, Sven; Zaal, Esther A.; Amaya Ramirez, Cinthia Claudia; Kowar, Alexander; Aviles-Huerta, Daniela; Berkers, Celia R.; Palm, Wilhelm; Tschaharganeh, Darjus; Krijgsveld, Jeroen; Loayza-Puch, Fabricio
- Abstract
Cellular senescence is characterized by a permanent growth arrest and is associated with tissue aging and cancer. Senescent cells secrete a number of different cytokines referred to as the senescence-associated secretory phenotype (SASP), which impacts the surrounding tissue and immune response. Here, we find that senescent cells exhibit higher rates of protein synthesis compared to proliferating cells and identify eIF5A as a crucial regulator of this process. Polyamine metabolism and hypusination of eIF5A play a pivotal role in sustaining elevated levels of protein synthesis in senescent cells. Mechanistically, we identify a p53-dependent program in senescent cells that maintains hypusination levels of eIF5A. Finally, we demonstrate that functional eIF5A is required for synthesizing mitochondrial ribosomal proteins and monitoring the immune clearance of premalignant senescent cells in vivo. Our findings establish an important role of protein synthesis during cellular senescence and suggest a link between eIF5A, polyamine metabolism, and senescence immune surveillance. Here the authors discovered that senescent cells increase protein synthesis through eIF5A regulation, involving polyamine metabolism and p53 pathways, crucial for immune surveillance and mitochondrial protein production in aging and cancer contexts.
- Subjects
PROTEIN synthesis; MITOCHONDRIAL proteins; RIBOSOMAL proteins; IMMUNE response; METABOLISM; CELLULAR aging; P53 protein
- Publication
Nature Communications, 2024, Vol 15, Issue 1, p1
- ISSN
2041-1723
- Publication type
Article
- DOI
10.1038/s41467-024-51901-w