Origin licensing and p53 status regulate Cdk2 activity during G(1). - Wikidata - wikimedia - TriplyDB

Origin licensing and p53 status regulate Cdk2 activity during G(1).

Origin licensing and p53 status regulate Cdk2 activity during G(1).

http://www.wikidata.org/entity/Q30434208

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Spatio-temporal regulation of the human licensing factor Cdc6 in replication and mitosis.Regulation and Function of Cdt1; A Key Factor in Cell Proliferation and Genome Stability A reduction of licensed origins reveals strain-specific replication dynamics in mice Successive phosphorylation of p27(KIP1) protein at serine-10 and C terminus crucially controls its potency to inactivate Cdk2 Recruitment of the human Cdt1 replication licensing protein by the loop domain of Hec1 is required for stable kinetochore-microtubule attachment Stress-stimulated mitogen-activated protein kinases control the stability and activity of the Cdt1 DNA replication licensing factor Cdk2 is required for p53-independent G2/M checkpoint control.DNA damage response and tumorigenesis in Mcm2-deficient mice Depletion of cellular pre-replication complex factors results in increased human cytomegalovirus DNA replication.Angiogenic factor signaling regulates centrosome duplication in endothelial cells of developing blood vessels Highly stable loading of Mcm proteins onto chromatin in living cells requires replication to unload Cell cycle proliferation decisions: the impact of single cell analyses.Mitotic UV irradiation induces a DNA replication-licensing defect that potentiates G1 arrest response.Cooperative effects of Akt-1 and Raf-1 on the induction of cellular senescence in doxorubicin or tamoxifen treated breast cancer cells.Chronic DNA Replication Stress Reduces Replicative Lifespan of Cells by TRP53-Dependent, microRNA-Assisted MCM2-7 Downregulation.Behavior of replication origins in Eukaryota - spatio-temporal dynamics of licensing and firing Role of dual specificity tyrosine-phosphorylation-regulated kinase 1B (Dyrk1B) in S-phase entry of HPV E7 expressing cells from quiescence Human papillomavirus E7 induces rereplication in response to DNA damage Diminished origin-licensing capacity specifically sensitizes tumor cells to replication stress.Divergent S phase checkpoint activation arising from prereplicative complex deficiency controls cell survival.Understanding the limitations of radiation-induced cell cycle checkpoints.How dormant origins promote complete genome replication.Mechanisms and pathways of growth failure in primordial dwarfism.Dormant origins, the licensing checkpoint, and the response to replicative stresses The contribution of dormant origins to genome stability: from cell biology to human genetics.Characterization, expression and silencing by RNAi of p53 from Penaeus monodon.Dormant origins as a built-in safeguard in eukaryotic DNA replication against genome instability and disease development.The High-Affinity Interaction between ORC and DNA that Is Required for Replication Licensing Is Inhibited by 2-Arylquinolin-4-Amines.The licensing checkpoint opens up.Spotlight on geminin.Rapid DNA replication origin licensing protects stem cell pluripotency.Mechanisms of Oncogene-Induced Replication Stress: Jigsaw Falling into Place.The Temporal Regulation of S Phase Proteins During G1.Lgr5+ intestinal stem cells reside in an unlicensed G1 phase.

P2860

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P2860

Origin licensing and p53 status regulate Cdk2 activity during G(1).

http://www.wikidata.org/entity/Q30434208

description

2009 nî lūn-bûn

@nan

2009 թուականի Յունիսին հրատարակուած գիտական յօդուած

@hyw

2009 թվականի հունիսին հրատարակված գիտական հոդված

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2009年の論文

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2009年論文

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2009年論文

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2009年論文

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2009年論文

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2009年論文

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2009年论文

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name

Origin licensing and p53 status regulate Cdk2 activity during G(1).

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Origin licensing and p53 status regulate Cdk2 activity during G(1).

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Origin licensing and p53 status regulate Cdk2 activity during G(1).

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Origin licensing and p53 status regulate Cdk2 activity during G(1).

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Origin licensing and p53 status regulate Cdk2 activity during G(1).

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Origin licensing and p53 status regulate Cdk2 activity during G(1).

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Origin licensing and p53 status regulate Cdk2 activity during G(1)

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Kathleen R Nevis

http://www.w3.org/2001/XMLSchema#string

Marila Cordeiro-Stone

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P2860

Inhibition of eukaryotic DNA replication by geminin binding to Cdt1

The ATM-Chk2-Cdc25A checkpoint pathway guards against radioresistant DNA synthesis

The regulated association of Cdt1 with minichromosome maintenance proteins and Cdc6 in mammalian cells

Chromatin association of human origin recognition complex, cdc6, and minichromosome maintenance proteins during the cell cycle: assembly of prereplication complexes in late mitosis

Preventing re-replication of chromosomal DNA.

Cell cycle analysis of the activity, subcellular localization, and subunit composition of human CAK (CDK-activating kinase)

Transforming growth factor-beta induces Cdk2 relocalization to the cytoplasm coincident with dephosphorylation of retinoblastoma tumor suppressor protein

Cdk phosphorylation triggers sequential intramolecular interactions that progressively block Rb functions as cells move through G1

Mouse geminin inhibits not only Cdt1-MCM6 interactions but also a novel intrinsic Cdt1 DNA binding activity

p21 is a universal inhibitor of cyclin kinases

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1952-1963

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scholarly article

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10.4161/CC.8.12.8811

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12

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8

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Jeanette Gowen Cook

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2009-06-21T00:00:00Z

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24425276

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19440053

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2972510

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