Crosstalk of the mitotic spindle assembly checkpoint with p53 to prevent polyploidy

Vogel, Celia; Kienitz, Anne; Hofmann, Irmgard; Müller, Rolf; Bastians, Holger

doi:10.1038/sj.onc.1207860

Cited by 144 publications

(144 citation statements)

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“…Under these conditions, the multinuclei contained a tetraploid DNA content as demonstrated by FACS analyses (Figure 2f). Furthermore, the premature exit from mitosis in spindle checkpoint deficient cells resulted in a similar high rate of endoreduplication in MAD1-kd and HCT-MAD2 þ /À cells (data not shown; Vogel et al, 2004a). Taken together, partial downregulation of either MAD1 or MAD2 results in a very similar functional inactivation of the spindle checkpoint.…”

Section: Partial Downregulation Of Mad1 or Mad2 Results In A Defectivesupporting

confidence: 48%

Partial downregulation of MAD1 causes spindle checkpoint inactivation and aneuploidy, but does not confer resistance towards taxol

et al. 2005

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The mitotic spindle assembly checkpoint ensures proper chromosome segregation during mitosis by inhibiting the onset of anaphase until all kinetochores are attached to the mitotic spindle and tension across the kinetochores is generated. Here, we report that the stable partial downregulation of the spindle checkpoint gene MAD1, which is observed in human cancer, leads to a functional inactivation of the spindle checkpoint resulting in gross aneuploidy. Interestingly, although Mad1 is thought to act as a kinetochore based activator of Mad2 during checkpoint activation, we show that normal levels of Mad2, but not of Mad1, are required for preventing premature sister chromatid separation and for maintaining the timing of an undisturbed mitosis, suggesting a Mad1 independent function of Mad2 that operates independent of its checkpoint function. Most significantly, a partial repression of either MAD1 or MAD2 confers resistance to nocodazole, a drug that inhibits microtubule attachment. In contrast, sensitivity to clinically relevant drugs like taxol or monastrol that inhibit the generation of tension across kinetochores is not modulated by partial downregulation of MAD1, suggesting a functional bifurcation of spindle checkpoint dependent apoptotic pathways.

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Section: Partial Downregulation Of Mad1 or Mad2 Results In A Defectivesupporting

confidence: 48%

Partial downregulation of MAD1 causes spindle checkpoint inactivation and aneuploidy, but does not confer resistance towards taxol

et al. 2005

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“…Mitotic slippage leads to the accumulation of postmitotic G1 cells, which are subsequently arrested in their cell cycle progression by activating a p53-dependent G1 checkpoint [37,38,39].…”

Section: Bis-demethoxycurcumin Triggers a Concurrent G1/s And Mitoticmentioning

confidence: 99%

Curcumin derivatives: Molecular basis of their anti-cancer activity

Basile

Ferrari

Lazzari

et al. 2009

Biochemical Pharmacology

164

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Curcumin, a phenolic compound from the plant Curcuma longa L., has shown a wide-spectrum of chemopreventive, anti-oxidant and anti-tumor properties. Although its promising chemotherapeutic activity, preclinical and clinical studies highlight Curcumin limited therapeutic application due to its instability in physiological conditions. To improve its stability and activity, many derivatives have been synthesized and studied, among which bis-DemethoxyCurcumin (bDMC) and diAcetylCurcumin (DAC). In this report, we show that both bDMC and DAC are more stable than Curcumin in physiological medium. To explore the mechanism of their chemotherapeutic effect, we studied their role in proliferation in the HCT116 human colon cancer cells. We correlated kinetic stability and cellular uptake data to their biological effects. Both bDMC and DAC impair correct spindles formation and induce a p53-and p21 CIP1/WAF1 -independent mitotic arrest, which is more stable and long-lasting for bDMC. A subsequent p53/p21 CIP1/WAF1 -dependent inhibition of G1 to S transition is triggered by Curcumin and DAC as a consequence of the mitotic slippage, preventing postmitotic cells from re-entering the cell cycle. Conversely, the G1/S arrest induced by bDMC is a direct effect of the drug and concomitant to the mitotic block. Finally, we demonstrate that bDMC induces rapid DNA double-strand breaks, moving for its possible development in anti-cancer clinical applications.

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“…Thus, although mitotic events (apoptosis and slippage) are p53-independent because the accumulated p53 cannot trans-activate during mitosis anyway, both post-mitotic apoptosis and G 1 arrest are p53-dependent, relying on Bax and p21, respectively. 6,60,[68][69][70][71][72] In summary, apoptosis-I and -II are drastically different: the former results from inhibition of transcription and the latter results from transcriptional rebound.…”

Section: Cells May Die In Mitosis or After The Slippage: Apoptosis-i mentioning

confidence: 99%

“…41,60,78 Perhaps, phosporylation of p53 causes its stabilization, during a transient mitotic arrest. 60 Thus, even before depletion of Mdm-2, phosphorylation of p53 may prevent p53 degradation. In addition, since most proteins are phosphorylated during mitosis, COP1 and Mdm-2 might be phosphorylated too.…”

Section: Mitotic Hyper-phosphorylationmentioning

confidence: 99%

“…57 Like inhibitors of transcription, microtubule active drugs (paclitaxel, vincristine, nocodazole), which cause mitotic inhibition of transcription, cause p53 accumulation. 10,41,[58][59][60][61] During mitotic arrest, p53 cannot induce its targets, because transcription is impossible. It was noticed that levels of p21 are decreased specifically during mitotic arrest despite an elevated levels of p53.…”

Section: Induction Of P53 By Inhibition Of Transcriptionmentioning

confidence: 99%

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Mitotic Arrest and Cell Fate: Why and How Mitotic Inhibition of Transcription Drives Mutually Exclusive Events

2007

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Crosstalk of the mitotic spindle assembly checkpoint with p53 to prevent polyploidy

Cited by 144 publications

References 31 publications

Partial downregulation of MAD1 causes spindle checkpoint inactivation and aneuploidy, but does not confer resistance towards taxol

Partial downregulation of MAD1 causes spindle checkpoint inactivation and aneuploidy, but does not confer resistance towards taxol

Curcumin derivatives: Molecular basis of their anti-cancer activity

Mitotic Arrest and Cell Fate: Why and How Mitotic Inhibition of Transcription Drives Mutually Exclusive Events

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