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- W2147246111 abstract "A proper DNA damage response (DDR), which monitors and maintains the genomic integrity, has been considered to be a critical barrier against genetic alterations to prevent tumor initiation and progression. The representative tumor suppressor p53 plays an important role in the regulation of DNA damage response. When cells receive DNA damage, p53 is quickly activated and induces cell cycle arrest and/or apoptotic cell death through transactivating its target genes implicated in the promotion of cell cycle arrest and/or apoptotic cell death such as p21(WAF1) , BAX, and PUMA. Accumulating evidence strongly suggests that DNA damage-mediated activation as well as induction of p53 is regulated by posttranslational modifications and also by protein-protein interaction. Loss of p53 activity confers growth advantage and ensures survival in cancer cells by inhibiting apoptotic response required for tumor suppression. RUNX family, which is composed of RUNX1, RUNX2, and RUNX3, is a sequence-specific transcription factor and is closely involved in a variety of cellular processes including development, differentiation, and/or tumorigenesis. In this review, we describe a background of p53 and a functional collaboration between p53 and RUNX family in response to DNA damage." @default.
- W2147246111 created "2016-06-24" @default.
- W2147246111 creator A5017785312 @default.
- W2147246111 creator A5034252509 @default.
- W2147246111 creator A5059436010 @default.
- W2147246111 date "2013-01-01" @default.
- W2147246111 modified "2023-10-02" @default.
- W2147246111 title "RUNX Family Participates in the Regulation of p53-Dependent DNA Damage Response" @default.
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