Survival responses of human embryonic stem cells to DNA damage

Filion, Tera M.; Qiao, Meng; Ghule, Prachi N.; Mandeville, Matthew; Wijnen, André J. van; Stein, Janet L.; Lian, Jane B.; Altieri, Dario C.

doi:10.1002/jcp.21735

Cited by 132 publications

(151 citation statements)

References 24 publications

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“…In principle, a lack of damage-induced checkpoint at the G1=S boundary would limit the time and resources available for DNA damage repair and compromise genomic integrity. However, mammalian ESC exhibit the robust induction of a DNA damage response that facilitates the elimination of damaged cells by apoptosis [4,37,44,50]. Consistent with previous reports [43], our results demonstrate that DNA damage response mechanisms in mESC include the recruitment of DNA repair components and the activation of gH2AX foci.…”

Section: Discussionsupporting

confidence: 88%

“…In these cells, the coordination of DNA damagesensing proteins and mediators of DNA damage check points would promote cell cycle arrest and allow the completion of HR before the cell enters G2 [49]. After externally induced DNA damage, and in common with teratocarcinoma cells, human and murine ESC traverse G1-phase progresses through S-phase and accumulate in at the G2=M boundary [4,37,44,50]. In principle, a lack of damage-induced checkpoint at the G1=S boundary would limit the time and resources available for DNA damage repair and compromise genomic integrity.…”

Section: Discussionmentioning

confidence: 99%

See 1 more Smart Citation

Homologous Recombination Conserves DNA Sequence Integrity Throughout the Cell Cycle in Embryonic Stem Cells

Serrano

Liang

Chang

et al. 2011

Stem Cells and Development

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Section: Discussionsupporting

confidence: 88%

Section: Discussionmentioning

confidence: 99%

Homologous Recombination Conserves DNA Sequence Integrity Throughout the Cell Cycle in Embryonic Stem Cells

Serrano

Liang

Chang

et al. 2011

Stem Cells and Development

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“…The function of p53-p21 axis has been studied by several groups in both mouse and human ESCs and in pluripotent human embryonal carcinoma cells using various strategies [10,[29][30][31][32]. Surprisingly, there have been many discrepancies between their findings, including differences in the ability of cells to transactivate the p21 gene or to produce increased levels of p21 protein when p21 transcripts are upregulated [10,[29][30][31]33]. When we examined p53 expression in hESCs with UVC-induced G1 delay, we found that at 3 hours after UVC irradiation, p53 protein is already dramatically increased, is phosphorylated on serines 15, 33, and 392, and localizes completely to cell nuclei.…”

Section: For the Experimental Design) (D-f)mentioning

confidence: 99%

“…Surprisingly, several studies have recently reported that hESCs fail to fully execute the G1/S checkpoint, which may account for the fast mitogenindependent (''automated'') progression of hESCs through G1 [8][9][10].…”

Section: Introductionmentioning

confidence: 99%

Human Embryonic Stem Cells Are Capable of Executing G1/S Checkpoint Activation

et al. 2010

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Embryonic stem cells progress very rapidly through the cell cycle, allowing limited time for cell cycle regulatory circuits that typically function in somatic cells. Mechanisms that inhibit cell cycle progression upon DNA damage are of particular importance, as their malfunction may contribute to the genetic instability observed in human embryonic stem cells (hESCs). In this study, we exposed undifferentiated hESCs to DNA-damaging ultraviolet radiation-C range (UVC) light and examined their progression through the G1/S transition. We show that hESCs irradiated in G1 phase undergo cell cycle arrest before DNA synthesis and exhibit decreased cyclin-dependent kinase two (CDK2) activity. We also show that the phosphatase Cdc25A, which directly activates CDK2, is downregulated in irradiated hESCs through the action of the checkpoint kinases Chk1 and/or Chk2. Importantly, the classical effector of the p53-mediated pathway, protein p21, is not a regulator of G1/S progression in hESCs. Taken together, our data demonstrate that cultured undifferentiated hESCs are capable of preventing entry into Sphase by activating the G1/S checkpoint upon damage to their genetic complement.

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“…Filion et al came to this conclusion as they did not observe increases in G1-phase cells after treatment of hES cells with -irradiation. They did, however, observe G2-arrest, indicating that G2/M checkpoint is functional (Filion et al 2009). In agreement with this, Sokolov et al observed a G2-arrest, but no G1-arrest after treatment of hES cells with 1Gy dose of X-rays (Sokolov et al 2011).…”

Section: Box 2: Human Embryonic Stem Cells and Induced Pluripotent Stmentioning

confidence: 99%