Literature DB >> 21354798

Regulation of cell differentiation by the DNA damage response.

Mara H Sherman1, Craig H Bassing, Michael A Teitell.   

Abstract

When faced with DNA double-strand breaks (DSBs), vertebrate cells activate DNA damage response (DDR) programs that preserve genome integrity and suppress malignant transformation. Three established outcomes of the DDR include transient cell cycle arrest coupled with DNA repair, apoptosis, or senescence. However, recent studies in normal and cancer precursor or stem cells suggest that a fourth potential outcome, cell differentiation, is under the influence of DDR programs. Here we review and discuss the emerging evidence that supports the linkage of signaling from DSBs to the regulation of differentiation, including some of the molecular mechanisms driving this under-appreciated DDR outcome. We also consider the physiologic and pathologic consequences of defects in DDR signaling on cell differentiation and malignant transformation.
Copyright © 2011 Elsevier Ltd. All rights reserved.

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Year:  2011        PMID: 21354798      PMCID: PMC3089693          DOI: 10.1016/j.tcb.2011.01.004

Source DB:  PubMed          Journal:  Trends Cell Biol        ISSN: 0962-8924            Impact factor:   20.808


  62 in total

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Journal:  Mol Cell Biol       Date:  1999-02       Impact factor: 4.272

5.  Activation of the ATM kinase by ionizing radiation and phosphorylation of p53.

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Review 6.  Cell cycle exit upon myogenic differentiation.

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7.  Second malignancy after treatment of pediatric Hodgkin disease.

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9.  DNA-PKcs: a T-cell tumour suppressor encoded at the mouse scid locus.

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  48 in total

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6.  DNA damage response in neonatal and adult stromal cells compared with induced pluripotent stem cells.

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7.  Interstitial telomeric repeats-associated DNA breaks.

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8.  NFκB regulates p21 expression and controls DNA damage-induced leukemic differentiation.

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9.  LKB1 inhibition of NF-κB in B cells prevents T follicular helper cell differentiation and germinal center formation.

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10.  Prolonged Mitosis of Neural Progenitors Alters Cell Fate in the Developing Brain.

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