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    Redox modulation of oxidatively-induced DNA damage by ascorbate enhances both in vitro and ex-vivo DNA damage formation and cell death in melanoma cells

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    Author
    Brown, Karen
    Saldanha, Gerald
    Sanusi, Timi
    Keyword
    Ascorbate
    Cell death
    Comet assay
    Malignant melanoma
    Oxidatively-induced DNA damage
    Date
    2024-03
    
    Metadata
    Show full item record
    DOI
    10.1016/j.freeradbiomed.2024.01.019
    Publisher's URL
    https://www.sciencedirect.com/science/article/pii/S0891584924000194?via%3Dihub
    Abstract
    Elevated genomic instability in cancer cells suggests a possible model-scenario for their selective killing via the therapeutic delivery of well-defined levels of further DNA damage. To examine this scenario, this study investigated the potential for redox modulation of oxidatively-induced DNA damage by ascorbate in malignant melanoma (MM) cancer cells, to selectively enhance both DNA damage and MM cell killing. DNA damage was assessed by Comet and ɣH2AX assays, intracellular oxidising species by dichlorofluorescein fluorescence, a key antioxidant enzymatic defence by assessment of catalase activity and cell survival was determined by clonogenic assay. Comet revealed that MM cells had higher endogenous DNA damage levels than normal keratinocytes (HaCaT cells); this correlated MM cells having higher intracellular oxidising species and lower catalase activity, and ranked with MM cell melanin pigmentation. Comet also showed MM cells more sensitive towards the DNA damaging effects of exogenous H2O2, and that ascorbate further enhanced this H2O2-induced damage in MM cells; again, with MM cell sensitivity to induced damage ranking with degree of cell pigmentation. Furthermore, cell survival data indicated that ascorbate enhanced H2O2-induced clonogenic cell death selectively in MM cells whilst protecting HaCaT cells. Finally, we show that ascorbate serves to enhance the oxidising effects of the MM therapeutic drug Elesclomol in both established MM cells in vitro and primary cell cultures ex vivo. Together, these results suggest that ascorbate selectively enhances DNA damage and cell-killing in MM cells. This raises the option of incorporating ascorbate into clinical oxidative therapies to treat MM.
    Citation
    Najeeb, H. A., Sanusi, T., Saldanha, G., Brown, K., Cooke, M. S., & Jones, G. D. (2024). Redox modulation of oxidatively-induced DNA damage by ascorbate enhances both in vitro and ex-vivo DNA damage formation and cell death in melanoma cells. Free radical biology & medicine, 213, 309–321. https://doi.org/10.1016/j.freeradbiomed.2024.01.019
    Type
    Article
    URI
    http://hdl.handle.net/20.500.12904/18281
    Collections
    Cancer
    Pathology

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