Differential DNA damage response and cell fate in human lung cells after exposure to genotoxic compounds

Líbalová, Helena; Závodná, Táňa; Margaryan, Hasmik; Milcová, Alena; Vrbová, Kristýna; Barošová, Hana; Červená, Tereza; Topinka, Jan; Rössner ml., Pavel

doi:https://dx.doi.org/10.1016/j.tiv.2023.105710

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Differential DNA damage response and cell fate in human lung cells after exposure to genotoxic compounds

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0581742 - ÚEM 2025 RIV GB eng J - Článek v odborném periodiku
Líbalová, Helena - Závodná, Táňa - Margaryan, Hasmik - Milcová, Alena - Vrbová, Kristýna - Barošová, Hana - Červená, Tereza - Topinka, Jan - Rössner ml., Pavel
Differential DNA damage response and cell fate in human lung cells after exposure to genotoxic compounds.
Toxicology in Vitro. Roč. 94, feb. (2024), č. článku 105710. ISSN 0887-2333. E-ISSN 1879-3177
Grant CEP: GA ČR(CZ) GJ18-06548Y; GA MŠMT(CZ) LM2023066; GA MŠMT(CZ) LM2023053; GA MŠMT(CZ) EF16_013/0001821; GA ČR(CZ) GJ18-06548Y
Institucionální podpora: RVO:68378041
Klíčová slova: genotoxicity * polycyclic aromatic hydrocarbons * anticancer drugs * DNA damage response * cell fate
Obor OECD: Public and environmental health
Impakt faktor: 3.2, rok: 2022
Způsob publikování: Open access
https://www.sciencedirect.com/science/article/pii/S0887233323001595?via%3Dihub

DNA damage can impair normal cellular functions and result in various pathophysiological processes including cardiovascular diseases and cancer. We compared the genotoxic potential of diverse DNA damaging agents, and focused on their effects on the DNA damage response (DDR) and cell fate in human lung cells BEAS-2B. Poly-cyclic aromatic hydrocarbons [PAHs, benzo[a]pyrene (B[a]P), 1-nitropyrene (1-NP)] induced DNA strand breaks and oxidative damage to DNA, anticancer drugs doxorubicin (DOX) and 5-bromo-2 '-deoxyuridine (BrdU) were less effective. DOX triggered the most robust p53 signaling indicating activation of DDR, followed by cell cycle arrest in the G2/M phase, induction of apoptosis and senescence, possibly due to the severe and irreparable DNA lesions. BrdU not only activated p53, but also increased the percentage of G1-phased cells and caused a massive accumulation of senescent cells. In contrast, regardless the activation of p53, both PAHs did not substantially affect the cell cycle distribution or senescence. Finally, a small fraction of cells accumulated only in the G2/M phase and exhibited increased cell death after the prolonged incubation with B[a]P. Overall, we characterized differential responses to diverse DNA damaging agents resulting in specific cell fate and highlighted the key role of DNA lesion type and the p53 signaling persistence.
Trvalý link: https://hdl.handle.net/11104/0350718

Počet záznamů: 1