Caspase-2-mediated cell death is required for deleting aneuploid cells

Dawar, Swati; Lim, Yoon Pin; Puccini, Joseph; White, Melissa; Thomas, Paul Q.; Bouchier‐Hayes, Lisa; Green, Douglas R.; Dorstyn, Loretta; Kumar, Sharad

doi:10.1038/onc.2016.423

Cited by 62 publications

(68 citation statements)

References 54 publications

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“…Importantly, cells from mice harboring catalytic-dead caspase-2 (CASP2 C320S ) also show increased aneuploidy following prolonged mitotic arrest 12 . These findings suggest that the activation and enzymatic activity of caspase-2 are required to mediate apoptosis of aneuploid cells.…”

Section: Introductionmentioning

confidence: 99%

Phosphorylation by Aurora B kinase regulates caspase-2 activity and function

Lim

Bellis

Sandow

et al. 2020

Preprint

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Mitotic catastrophe (MC) is an important oncosuppressive mechanism that serves to eliminate cells that become polyploid or aneuploidy due to aberrant mitosis. Previous studies have demonstrated that the activation and catalytic function of caspase-2 are key steps in MC to trigger apoptosis and/or cell cycle arrest of mitotically defective cells. However, the molecular mechanisms that regulate caspase-2 activation and its function are unclear. Here we identify six new phosphorylation sites in caspase-2 and show that a key mitotic kinase, Aurora B kinase (AURKB), phosphorylates caspase-2 at the highly conserved residue S384. We demonstrate that phosphorylation at S384 blocks caspase-2 catalytic activity and apoptosis function in response to mitotic insults, without affecting caspase-2 dimerisation. Moreover, molecular modelling suggests that phosphorylation at S384 may affect substrate binding by caspase-2. We propose that caspase-2 S384 phosphorylation by AURKB is a key mechanism that controls caspase-2 activation during mitosis.

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Section: Introductionmentioning

confidence: 99%

Phosphorylation by Aurora B kinase regulates caspase-2 activity and function

Lim

Bellis

Sandow

et al. 2020

Preprint

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“…16 Dawar et al performed time-lapse imaging and cytogenetic analyses of primary splenocytes from Casp2 ¡/¡ mice and CASP2-depleted human cancer cells to show that the absence of CASP2 promoted mitotic slippage as well as the survival of the resulting multinucleated cells that were able to resume proliferation in clonogenic assays. These results suggest that CASP2 may also contribute to SAC signaling, an intriguing hypothesis that requires further confirmation.…”

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confidence: 99%

“…13 Three recent studies shed light on the mechanism of, and the signal responsible for, CASP2 activation during mitotic catastrophe unveiling the existence of a tight connection between CASP2 and the p53 pathway. [14][15][16] By analyzing colorectal cancers and cell lines displaying high levels of CIN, either at the baseline or upon the pharmacological abrogation of the SAC or increase of replication stress, Lopez-Garcia and colleagues identified a novel mechanism of tolerance to non-diploidy based on the downregulation of CASP2 expression.…”

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confidence: 99%

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Caspase 2 in mitotic catastrophe: The terminator of aneuploid and tetraploid cells

Vitale

Manic

Castedo

et al. 2017

Molecular & Cellular Oncology

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Mitotic catastrophe is an oncosuppressive mechanism that targets cells experiencing defective mitoses via the activation of specific cell cycle checkpoints, regulated cell death pathways and/or cell senescence. This prevents the accumulation of karyotypic aberrations, which otherwise may drive oncogenesis and tumor progression. Here, we summarize experimental evidence confirming the role of caspase 2 (CASP2) as the main executor of mitotic catastrophe, and we discuss the signals that activate CASP2 in the presence of mitotic aberrations. In addition, we summarize the main p53-dependent and -independent effector pathways through which CASP2 limits chromosomal instability and non-diploidy, hence mediating robust oncosuppressive functions.

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“…NPM1 and caspase-2 driven apoptosis from the nucleolus could also play a key role in this process, since Kumar and colleagues recently showed that caspase-2 induces apoptosis to remove aneuploid cells. 6 Continued efforts to unravel the contributions of the nucleolar complex to apoptosis or regulation of proliferation will be imperative to determining how caspase-2 protects from aneuploidy.…”

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confidence: 99%