CARF is a multi-module regulator of cell proliferation and a molecular bridge between cellular senescence and carcinogenesis
- PMID: 28754531
- DOI: 10.1016/j.mad.2017.07.008
CARF is a multi-module regulator of cell proliferation and a molecular bridge between cellular senescence and carcinogenesis
Abstract
CARF (Collaborator of ARF) was first identified as an ARF (Alternative Reading Frame, p14ARF)-interacting protein in a yeast two-hybrid interactive screening. Subsequently, it was shown to stabilize the p53-tumor suppressor protein in an ARF-dependent or -independent manner. It acts as a transcriptional repressor of HDM2 that exerts a negative feedback on p53 by its proteasomal-mediated degradation. CARF-driven control over p53-HDM2-p21WAF1 axis was shown to regulate cell proliferative fates. Cells with CARF-overexpression (CARF-OE) and superexpression (CARF-SE) showed growth arrest and pro-proliferative phenotypes, respectively. On the other hand, apoptosis was triggered in CARF-compromised cells. In the present review, we provide a comprehensive current understanding into the molecular mechanisms of CARF functions in regulation of DNA damage response, cell cycle checkpoints, cell survival and death signaling pathways. We discuss how thresh-hold of CARF level determines fate of cells to senescence and malignant transformation.
Keywords: CARF; Malignant transformation; Overexpression; Senescence; Superexpression.
Copyright © 2017 Elsevier B.V. All rights reserved.
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