Disregulation of mitotic checkpoints and regulatory proteins following acute expression of SV40 large T antigen in diploid human cells

Chang, Ted Hung-Tse; Ray, F. Andrew; Da, Thompson; Schlegel, Richard

doi:10.1038/sj.onc.1201196

Cited by 78 publications

(68 citation statements)

References 46 publications

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“…Taken together, our observations therefore demonstrate that SV-LT abrogates repression of the cdc25C promoter which is fully consistent with the genomic footprinting data showing a loss of CDF-DNA interaction. Our observations are also in agreement with published data showing that SV-LT expressing cells contain elevated levels of Cdc25C (Chang et al, 1997).…”

supporting

confidence: 94%

“…The transcriptional deregulation of cell cycle genes appears to be a major strategy employed by the oncoproteins of DNA tumor viruses to override growth control mechanisms in mammalian cells (Buchou et al, 1993;Oshima et al, 1993;Spitkovsky et al, 1994;Cheng et al, 1995;Schulze et al, 1995;Chang et al, 1997). Oncoproteins, including the adenovirus E1a gene product, the SV40 large T antigen (SV-LT), and the human papilloma virus E7 protein, bind pocket proteins through regions which are necessary for transformation (DeCaprio et al, 1989;Dyson et al, 1989).…”

mentioning

confidence: 99%

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The SV40 large T oncoprotein disrupts DNA-binding of the cell cycle-regulated transcriptional repressor CDF

1999

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A hallmark of neoplastic transformation by DNA tumor viruses is the deregulation of cell cycle genes. At least in some genes, this deregulation appears to be due to the oncoprotein-mediated disruption of complexes between E2F and pocket proteins and the ensuing generation of transcriptionally active free E2F. In the present study, we have analysed the e ect of the SV40 large T oncoprotein (SV-LT) on the function of a di erent cell cycle-regulated transcriptional repressor, CDF, which is the principal regulator of the cdc25C, cyclin A and cdc2 genes. As shown by genomic footprinting of sorted G 1 and G 2 cell populations, transformation by SV-LT completely abrogated protection of the CDF binding site (CDE-CHR) in the cdc25C promoter. In agreement with this observation, expression of the SV-LT in ®broblasts led to a dramatic up-regulation of the cdc25C promoter in cells synchronized in G 0 . These ®ndings indicate that the oncoprotein-mediated dissociation of the CDF repressor protein from its cognate DNA-binding site is a major mechanism in virus-induced transcriptional deregulation.

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supporting

confidence: 94%

mentioning

confidence: 99%

The SV40 large T oncoprotein disrupts DNA-binding of the cell cycle-regulated transcriptional repressor CDF

1999

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“…The apparent copy number independence of WRN function in our experiments may reflect the comparatively high level of WRN protein in fibroblast cell lines [27] and/or attenuated DNA damage checkpoint functioning in SV40-transformed fibroblast cell lines (see, e.g. [28]). Fig.…”

Section: Resultsmentioning

confidence: 75%

The Werner syndrome protein has separable recombination and survival functions☆

et al. 2004

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The Werner syndrome (WS) protein WRN is unique in possessing a 3 to 5 exonuclease activity in addition to the 3 to 5 helicase activity characteristic of other RecQ proteins. In order to determine in vivo functions of the WRN catalytic activities and their roles in Werner syndrome pathogenesis, we quantified cell survival and homologous recombination after DNA damage in cells expressing WRN missense-mutant proteins that lacked exonuclease and/or helicase activity. Both WRN biochemical activities were required to generate viable recombinant daughter cells. In contrast, either activity was sufficient to promote cell survival after DNA damage in the absence of recombination. These results indicate that WRN has recombination and survival functions that can be separated by missense mutations. Two implications are that Werner syndrome most likely results from the loss of both activities and their associated functions from patient cells, and that WRN missense mutations or polymorphisms could promote genetic instability and cancer in the general population by selectively interfering with recombination in somatic cells.

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“…Since both oncogenic Ras and oncogenic Raf will cause potent activation of the MAP kinase cascade, these data would initially appear to be in conflict with our results. However, because these hepatocyte cell lines were immortalized with SV40 virus the function of p53 may have been compromised, and p53 function has been demonstrated to be one mechanism by which cells can induce expression of p21 Cip-" [40][41][42]. Thus it is probable that SV40 transformation of these hepatocyte cell lines may have made these cells incompetent to induce p21 Cip-" via chronic activation of the MAP kinase cascade.…”

Section: Discussionmentioning

confidence: 99%

The mitogen-activated protein (MAP) kinase cascade can either stimulate or inhibit DNA synthesis in primary cultures of rat hepatocytes depending upon whether its activation is acute/phasic or chronic

Tombes

Auer

Mikkelsen

et al. 1998

Biochemical Journal

179

155

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Bailie et al. [In Vitro Cell Dev. Biol. (1992) 28A, 621-624] reported that primary cultures of rat hepatocytes possess low affinity binding sites for nerve growth factor (NGF). NGF treatment of primary cultures of rat hepatocytes with a maximally effective concentration of NGF (20 ng/ml, 0.8 nM) caused acute phasic activation of Raf-1 and p42MAPkinase, and a smaller sustained activation of B-Raf. The transient increase in Raf-1 and p42MAPkinase activity returned to baseline within ~ 30 min. NGF treatment of hepatocytes did not induce expression of cyclin dependent kinase (cdk) inhibitor proteins, but instead stimulated cdk2 activity and increased [3H]thymidine incorporation into DNA. In contrast to hepatocytes, NGF treatment of PC12 pheochromocytoma cells caused large sustained activations of B-Raf and p42MAPkinase, and a lower phasic activation of Raf-1. The sustained activations of B-Raf and p42MAPkinase were for more than 5 h. Treatment of PC12 cells with NGF increased p21Cip1/WAF-1 expression, reduced cdk2 activity and inhibited DNA synthesis, the opposite to the effects of NGF treatment of hepatocytes. However when p42MAPkinase was chronically activated in hepatocytes, via infection with an inducible oestrogen receptor-Raf-1 fusion protein, expression of p21Cip-1/WAF1 and p16INK4a cdk inhibitor proteins increased, cdk2 activity decreased, and DNA synthesis decreased. Equally, treatment of hepatocytes with 50 mM ethanol elevated the basal activity of p42MAPkinase and temporally extended the ability of NGF treatment to activate p42MAPkinase. Ethanol and NGF co-treatment increased expression of p21Cip-1/WAF1 and p16INK4a cdk inhibitor proteins and decreased hepatocyte DNA synthesis. These data demonstrate that NGF can cause either acute/phasic or sustained activation of the MAP kinase cascade in different cell types. Acute activation of the MAP kinase cascade correlated with increased DNA synthesis. In contrast, sustained activation of the MAP kinase cascade correlated with increased expression of cdk inhibitor proteins, a reduction in cdk activity, and an inhibition of DNA synthesis. These data suggest a general mechanism exists where acute activation of the MAP kinase cascade promotes G1 progression/S phase entry and that chronic activation of the MAP kinase cascade inhibits this process.

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Disregulation of mitotic checkpoints and regulatory proteins following acute expression of SV40 large T antigen in diploid human cells

Cited by 78 publications

References 46 publications

The SV40 large T oncoprotein disrupts DNA-binding of the cell cycle-regulated transcriptional repressor CDF

The SV40 large T oncoprotein disrupts DNA-binding of the cell cycle-regulated transcriptional repressor CDF

The Werner syndrome protein has separable recombination and survival functions☆

The mitogen-activated protein (MAP) kinase cascade can either stimulate or inhibit DNA synthesis in primary cultures of rat hepatocytes depending upon whether its activation is acute/phasic or chronic

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