| Literature DB >> 28822913 |
Samuel Bru1, Bàrbara Samper-Martín1, Eva Quandt1, Sara Hernández-Ortega1, Joan M Martínez-Laínez1, Eloi Garí2, Marta Rafel2, Javier Torres-Torronteras3, Ramón Martí3, Mariana P C Ribeiro1, Javier Jiménez4, Josep Clotet5.
Abstract
Cells require extra amounts of dNTPs to repair DNA after damage. Polyphosphate (polyP) is an evolutionary conserved linear polymer of up to several hundred inorganic phosphate (Pi) residues that is involved in many functions, including Pi storage. In the present article, we report on findings demonstrating that polyP functions as a source of Pi when required to sustain the dNTP increment essential for DNA repair after damage. We show that mutant yeast cells without polyP produce less dNTPs upon DNA damage and that their survival is compromised. In contrast, when polyP levels are ectopically increased, yeast cells become more resistant to DNA damage. More importantly, we show that when polyP is reduced in HEK293 mammalian cell line cells and in human dermal primary fibroblasts (HDFa), these cells become more sensitive to DNA damage, suggesting that the protective role of polyP against DNA damage is evolutionary conserved. In conclusion, we present polyP as a molecule involved in resistance to DNA damage and suggest that polyP may be a putative target for new approaches in cancer treatment or prevention.Entities:
Keywords: DNA damage; Human dermal fibroblasts; Mammalian cells; Polyphosphate; Repair; Saccharomyces
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Year: 2017 PMID: 28822913 DOI: 10.1016/j.dnarep.2017.08.001
Source DB: PubMed Journal: DNA Repair (Amst) ISSN: 1568-7856