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    Deregulation of cell growth and apoptosis in UV-induced melanomagenesis

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    Deregulation of cell growth and apoptosis in UV-induced melanomagenesis.pdf (833.8Kb)
    Date
    2020
    Author
    Ouhtit A.
    Gupta I.
    Gaur R.L.
    Fernando A.
    Abd El-Azim A.O.
    Eid A.
    Becker T.M.
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    Abstract
    We have previously characterized the role of p16/Rb in coordinating the early events in UVB-irradiated skin. As an extension to this work, normal melanocytes and mutant p16-inducible melanoma cell models were employed to elucidate further the coordinated molecular mechanisms occurring during early UVB exposure. Our results showed that melanocytes expressed p16 only at a high UVB dose, with undetectable p53. The Bax/Bcl2 ratio increased at higher dose, indicating that the cells had selected apoptosis program. In the wt-p16 melanoma cells, while low UVB dose upregulated p16, the high dose suppressed it, and further abrogated Cdk6 but not Cdk4. Interestingly, while induction of mutant-p16 increased Cdk4, cdk6 and pRb proteins, UVB exposure did not affect this increase. More interestingly, p16 mutant cells increased their resistance to apoptosis at high UVB-dose, associated with decreased Bax and increased Bcl2 expression. Thus, mutant-p16 appears to dictate a deregulation of cell cycle and increased resistance to apoptosis in melanoma cells. Together, the data indicate a deregulation of p16INK4/Rb pathway as an early event in UVB-induced melanomagenesis. 2020 Frontiers in Bioscience. All rights reserved.
    DOI/handle
    http://dx.doi.org/10.2741/E868
    http://hdl.handle.net/10576/40020
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