Literature DB >> 17565509

DNA-damage response network at the crossroads of cell-cycle checkpoints, cellular senescence and apoptosis.

Estelle Schmitt1, Claudie Paquet, Myriam Beauchemin, Richard Bertrand.   

Abstract

Tissue homeostasis requires a carefully-orchestrated balance between cell proliferation, cellular senescence and cell death. Cells proliferate through a cell cycle that is tightly regulated by cyclin-dependent kinase activities. Cellular senescence is a safeguard program limiting the proliferative competence of cells in living organisms. Apoptosis eliminates unwanted cells by the coordinated activity of gene products that regulate and effect cell death. The intimate link between the cell cycle, cellular senescence, apoptosis regulation, cancer development and tumor responses to cancer treatment has become eminently apparent. Extensive research on tumor suppressor genes, oncogenes, the cell cycle and apoptosis regulatory genes has revealed how the DNA damage-sensing and -signaling pathways, referred to as the DNA-damage response network, are tied to cell proliferation, cell-cycle arrest, cellular senescence and apoptosis. DNA-damage responses are complex, involving "sensor" proteins that sense the damage, and transmit signals to "transducer" proteins, which, in turn, convey the signals to numerous "effector" proteins implicated in specific cellular pathways, including DNA repair mechanisms, cell-cycle checkpoints, cellular senescence and apoptosis. The Bcl-2 family of proteins stands among the most crucial regulators of apoptosis and performs vital functions in deciding whether a cell will live or die after cancer chemotherapy and irradiation. In addition, several studies have now revealed that members of the Bcl-2 family also interface with the cell cycle, DNA repair/recombination and cellular senescence, effects that are generally distinct from their function in apoptosis. In this review, we report progress in understanding the molecular networks that regulate cell-cycle checkpoints, cellular senescence and apoptosis after DNA damage, and discuss the influence of some Bcl-2 family members on cell-cycle checkpoint regulation.

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Year:  2007        PMID: 17565509      PMCID: PMC1879163          DOI: 10.1631/jzus.2007.B0377

Source DB:  PubMed          Journal:  J Zhejiang Univ Sci B        ISSN: 1673-1581            Impact factor:   3.066


  312 in total

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Journal:  Cell       Date:  1993-08-27       Impact factor: 41.582

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Journal:  Cancer Res       Date:  1993-09-15       Impact factor: 12.701

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8.  bcl-x, a bcl-2-related gene that functions as a dominant regulator of apoptotic cell death.

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Journal:  Cell       Date:  1993-08-27       Impact factor: 41.582

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Authors:  E Solary; R Bertrand; J Jenkins; Y Pommier
Journal:  Exp Cell Res       Date:  1992-12       Impact factor: 3.905
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4.  Phospho-Bcl-x(L)(Ser62) plays a key role at DNA damage-induced G(2) checkpoint.

Authors:  Jianfang Wang; Myriam Beauchemin; Richard Bertrand
Journal:  Cell Cycle       Date:  2012-06-01       Impact factor: 4.534

5.  Mahanine, a novel mitochondrial complex-III inhibitor induces G0/G1 arrest through redox alteration-mediated DNA damage response and regresses glioblastoma multiforme.

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6.  Parvovirus infection-induced DNA damage response.

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Journal:  Future Virol       Date:  2013-03-01       Impact factor: 1.831

7.  Function and regulation mechanism of Chk1 during meiotic maturation in porcine oocytes.

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9.  Association and impact of XPG Asp 1104 His gene polymorphism in HIV 1 disease progression to AIDS among north Indian HIV seropositive individuals.

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10.  Effects on DNA Damage and/or Repair Processes as Biological Mechanisms Linking Psychological Stress to Cancer Risk.

Authors:  Frank J Jenkins; Bennett Van Houten; Dana H Bovbjerg
Journal:  J Appl Biobehav Res       Date:  2014-02-01
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