Coordinated Activation of the Origin Licensing Factor CDC6 and CDK2 in Resting Human Fibroblasts Expressing SV40 Small T Antigen and Cyclin E

Sotillo, Elena; Garriga, Judit; Padgaonkar, Amol; Kurimchak, Alison; Cook, Jeanette Gowen; Graña, Xavier

doi:10.1074/jbc.m900687200

Cited by 13 publications

(13 citation statements)

References 41 publications

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“…30,31 The methionine stress-induced drop in Cdc6 predicted a corresponding loss in phosphorylation of Thr160 on Cdk2, resulting in lowered kinase activity, which we observed. Our data confirms Cdk2 kinase inactivation during methionine stress in MDAMB468 cells, and suggests that loss of Cdk2 activity might contribute to the observed G 1 /S cell cycle arrest.…”

Section: Methodsmentioning

confidence: 55%

Downregulation of Cdc6 and pre-replication complexes in response to methionine stress in breast cancer cells

et al. 2012

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Section: Methodsmentioning

confidence: 55%

Downregulation of Cdc6 and pre-replication complexes in response to methionine stress in breast cancer cells

et al. 2012

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“…In our hands these cells have proliferation properties similar to those exhibited by parental non-immortal BJ fibroblasts [22,23]. To eliminate the effects of transduction as a cause of differential effects in gene expression, all cells were transduced identically using the inducible Adeno-X™ Tet-Off system from Clontech carrying a dnCDK9 transgene under a tetracycline repressible promoter.…”

Section: Resultsmentioning

confidence: 99%

CDK9 inhibition strategy defines distinct sets of target genes

Garriga¹,

Graña

2014

BMC Res Notes

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BackgroundCDK9 is the catalytic subunit of the Positive Transcription Elongation Factor b (P-TEFb), which phosphorylates the CTD of RNAPII and negative elongation factors enabling for productive elongation after initiation. CDK9 associates with T-type cyclins and cyclin K and its activity is tightly regulated in cells at different levels. CDK9 is also the catalytic subunit of TAK (Tat activating Kinase), essential for HIV1 replication. Because of CDK9′s potential as a therapeutic target in AIDS, cancer, inflammation, and cardiomyophathy it is important to understand the consequences of CDK9 inhibition. A previous gene expression profiling study performed with human glioblastoma T98G cells in which CDK9 activity was inhibited either with a dominant negative mutant form of CDK9 (dnCDK9) or the pharmacological inhibitor Flavopiridol unveiled striking differences in gene expression effects. In the present report we extended these studies by (1) using both immortalized normal human fibroblasts and primary human astrocytes, (2) eliminating potential experimental variability due to transduction methodology and (3) also modulating CDK9 activity with siRNA.FindingsStriking differences in the effects on gene expression resulting from the strategy used to inhibit CDK9 activity (dnCDK9 or FVP) remain even when potential variability due to viral transduction is eliminated. siRNA mediated CDK9 knockdown in human fibroblasts and astrocytes efficiently reduced CDK9 expression and led to potent changes in gene expression that exhibit little correlation with the effects of dnCDK9 or FVP. Interestingly, HEXIM1 a validated CDK9 target gene, was found to be potently downregulated by dnCDK9, FVP and siCDK9, but the cluster of genes with expression profiles similar to HEXIM1 was small. Finally, cluster analysis of all treatments revealed higher correlation between treatments than cell type origin.ConclusionThe nature of the strategy used to inhibit CDK9 profoundly affects the patterns of gene expression resulting from CDK9 inhibition. These results suggest multiple variables that affect outcome, including kinetics of inhibition, potency, off-target effects, and selectivity issues. This is particularly important when considering CDK9 as a potential target for therapeutic intervention.

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“…In the late G1 phase, CDK2 is activated by its association with cyclin E and phosphorylates retinoblastoma protein (Rb), resulting in the release of E2F transcription factor, inducing transcriptional activation of genes required for S-phase progression and DNA replication, leading to passage from G1/S phase to S phase (Berthet et al, 2006; Merrick et al, 2011). CDK2 also phosphorylates DNA replication factors to facilitate pre-RC assembly and origin firing (Sotillo et al, 2009). In S phase, CDK2 associates with cyclin A, which is required for the S-phase completion.…”

Section: Discussionmentioning

confidence: 99%