The Chk1-mediated S-phase Checkpoint Targets Initiation Factor Cdc45 via a Cdc25A/Cdk2-independent Mechanism

Liu, Peijun; Barkley, Laura R.; Day, Tovah; Bi, Xin; Slater, Damien; Alexandrow, Mark G.; Nasheuer, Heinz-Peter; Vaziri, Cyrus

doi:10.1074/jbc.m602982200

Cited by 84 publications

(104 citation statements)

References 59 publications

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“…30 Average labeled fiber lengths obtained in these experiments were 34.9 kb (n = 497) and 35.59 kb (n = 380) for siCon-and correlates with inhibition of DNA synthesis when the S-phase checkpoint is active. 26 Taken together, our data show association of FANCD2 with Cdc45 in the chromatin concomitant with DNA replication. These results are consistent with a potential role for FANCD2 in promoting efficient chromatin loading of Cdc45 and facilitating initiation and/or elongation stages of DNA synthesis.…”

supporting

confidence: 49%

“…Rat anti-Cdc45 monoclonal antibody has been described previously. 26 Antibodies against Cdc6 (sc-9964), Cdk2 (sc-163), Cdk4 (sc-260), Chk1 (sc-7898), Cyclin A (sc-596), FANCL (sc-66887).…”

Section: Methodsmentioning

confidence: 99%

“…2,6,21 H1299 human lung carcinoma cells were chosen for these initial experiments, because we and others have characterized cell cycle events and DNA replication parameters extensively in this line. [22][23][24][25][26] We achieved efficient ablation of FANCD2 expression in exponentially-growing H1299 cells as shown by immunoblotting (Fig. 1A).…”

Section: Fancd2-deficiency Affects Cell Cycle Progressionmentioning

confidence: 99%

“…The association of Cdc45 with chromatin and pre-RC components is negatively regulated by the Chk1-mediated S-phase checkpoint in a CDK2-independent manner. 26 Interestingly, the association of FANCD2 with Cdc45 on chromatin was also reduced by approximately 32% following genotoxin (BPDE)-treatment under conditions of S-phase checkpoint activation (Fig. 4B).…”

mentioning

confidence: 99%

“…However, a 50% inhibition of DNA synthesis resulting from reduced elongation in genotoxin-treated cells is readily detectable by velocity sedimentation. 26 Therefore, any putative changes in rates of fork progression due to FANCD2-deficiency are likely to be very modest. Alternatively, it is possible that FANCD2-deficiency only affects elongation of a subset of replicons and does not affect the elongation stage of DNA synthesis globally.…”

mentioning

confidence: 99%

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A novel role for fanconi anemia (FA) pathway effector protein FANCD2 in cell cycle progression of untransformed primary human cells

Song¹,

Barkley²,

Day³

et al. 2010

Cell Cycle

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supporting

confidence: 49%

“…Rat anti-Cdc45 monoclonal antibody has been described previously. 26 Antibodies against Cdc6 (sc-9964), Cdk2 (sc-163), Cdk4 (sc-260), Chk1 (sc-7898), Cyclin A (sc-596), FANCL (sc-66887).…”

Section: Methodsmentioning

confidence: 99%

Section: Fancd2-deficiency Affects Cell Cycle Progressionmentioning

confidence: 99%

mentioning

confidence: 99%

mentioning

confidence: 99%

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A novel role for fanconi anemia (FA) pathway effector protein FANCD2 in cell cycle progression of untransformed primary human cells

Song¹,

Barkley²,

Day³

et al. 2010

Cell Cycle

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The dynamic replicon: adapting to a changing cellular environment

Herrick

2010

BioEssays

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Eukaryotic cells are often exposed to fluctuations in growth conditions as well as endogenous and exogenous stress-related agents. During development, global patterns of gene transcription change substantially, and these changes are associated with altered patterns of DNA replication and larger distances between replication origins in somatic cells compared to embryos. Conversely, when cells experience difficulties while replicating DNA, the replication program is dramatically altered and distances between replication origins decrease. Recent evidence indicates that each unit of replication, or replicon, can correspond to one or more potential replication origins, but in the case of multiple potential origins, only one is selected to initiate replication of the replicon. How one origin is selected from multiple potential origins and how origin densities are regulated during genome duplication remains unclear. The following review addresses some of the mechanisms involved in regulating replication origins during both a normal and perturbed eukaryotic cell cycle.

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Roles of Chk1 in cell biology and cancer therapy

Zhang

Hunter

2013

Intl Journal of Cancer

384

359

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The evolutionally conserved DNA damage response (DDR) and cell cycle checkpoints preserve genome integrity. Central to these genome surveillance pathways is a protein kinase, Chk1. DNA damage induces activation of Chk1, which then transduces the checkpoint signal and facilitates cell cycle arrest and DNA damage repair. Significant progress has been made recently towards our understanding of Chk1 regulation and its implications in cancer etiology and therapy. Specifically, a model that involves both spatiotemporal and conformational changes of proteins has been proposed for Chk1 activation. Further, emerging evidence suggests that Chk1 does not appear to be a tumor suppressor; instead, it promotes tumor growth and may contribute to anticancer therapy resistance. Recent data from our laboratory suggest that activating, but not inhibiting, Chk1 in the absence of chemotherapy might represent an innovative approach to suppress tumor growth. These findings suggest unique regulation of Chk1 in cell biology and cancer etiology, pointing to novel strategies for targeting Chk1 in cancer therapy.

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The Chk1-mediated S-phase Checkpoint Targets Initiation Factor Cdc45 via a Cdc25A/Cdk2-independent Mechanism

Cited by 84 publications

References 59 publications

A novel role for fanconi anemia (FA) pathway effector protein FANCD2 in cell cycle progression of untransformed primary human cells

A novel role for fanconi anemia (FA) pathway effector protein FANCD2 in cell cycle progression of untransformed primary human cells

The dynamic replicon: adapting to a changing cellular environment

Roles of Chk1 in cell biology and cancer therapy

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