The Aurora Kinase Inhibitor VX-680 Induces Endoreduplication and Apoptosis Preferentially in Cells with Compromised p53-Dependent Postmitotic Checkpoint Function

Gizatullin, Farid; Yao, Yao; Kung, Victor; Harding, Matthew W.; Loda, Massimo; Shapiro, Geoffrey I.

doi:10.1158/0008-5472.can-05-3353

Cited by 168 publications

(183 citation statements)

References 34 publications

(47 reference statements)

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“…We also exclude three additional protein kinases involved in mitosis as targets for this compound. Interestingly, Aurora A-like inhibitory phenotypes have not previously been reported in cells exposed to VX-680, 15,30 but we now demonstrate phenotypes consistent with inhibition of Aurora A in human cells exposed to the drug, including the appearance of monopolar spindles in mitotic cells, and the suppression of phosphorylation events that are attributable to the inhibition of Aurora A activity. Similar Aurora A-like inhibitory phenotypes have recently been reported with chemically distinct inhibitors of the Aurora kinases, including ZM3 18 and MLN8054, 19 and these findings are all in close agreement with the mitotic phenotype seen in two model eukaryotic organisms, where loss of Aurora A induces a centrosome separation defect and a monopolar spindle phenotype.…”

Section: Discussionsupporting

confidence: 63%

“…Prolonged treatment of either HeLa or DLD-1 cells with VX-680 for several days led to the accumulation of polyploid cells and loss of viability, as detected by flow cytometry, consistent with published data with this compound. 16,30 To help clarify the effects of VX-680 on mitosis, we analysed living human DLD-1 cells stably expressing Histone H2B-GFP by time-lapse fluorescence microscopy. Supplementary Movies 1 and 2 document the effects of DMSO or VX-680 on these cells.…”

Section: © 2 0 0 7 L a N D E S B I O S C I E N C E D O N O T D I S mentioning

confidence: 99%

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VX-680 Inhibits Aurora A and Aurora B Kinase Activity in Human Cells

Tyler¹,

Shpiro²,

Marquez³

et al. 2007

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Section: Discussionsupporting

confidence: 63%

Section: © 2 0 0 7 L a N D E S B I O S C I E N C E D O N O T D I S mentioning

confidence: 99%

VX-680 Inhibits Aurora A and Aurora B Kinase Activity in Human Cells

Tyler¹,

Shpiro²,

Marquez³

et al. 2007

Cell Cycle

107

100

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“…The Aurora kinases represent one such class of molecular targets that are essential for progression through mitosis, and small molecule inhibitors of these kinases possess broad antitumor efficacy that has not yet been shown to discriminate on a cancer genetic basis. 7,11 Although it has been demonstrated that cancer cells deficient in p53 show accelerated polyploidization when treated with VX-680, 23 this does not appear to represent genetic susceptibility per se as cells harboring wild-type p53 are also subject to polyploidization-mediated cell death, though perhaps with delayed kinetics. Our data provide genetic evidence to indicate that the Aurora kinase inhibitor, AZD1152, which is currently undergoing clinical evaluation and potentially of another clinical compound, VX-680, may be relatively ineffective in tumor cells that overexpress MDR1 or BCRP.…”

Section: Discussionmentioning

confidence: 99%

Identification of genes that confer tumor cell resistance to the Aurora B kinase inhibitor, AZD1152

et al. 2009

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“…9 VX-680 inhibits aurora A and B kinases with low nanomolar potency 11 and the cellular effects are consistent with the inhibition of both aurora A and B kinases, that is, monospindle phenotype, disruption of spindle assembly checkpoint (SAC), aberrant chromosomal segregation, endoreduplication and cytokinesis failure. 12,13 Endoreduplication, the re-replication of DNA in the absence of mitotic division, ultimately results in polyploidy and cell death. It is thought that a p53-dependent postmitotic checkpoint prevents polyploidy.…”

mentioning

confidence: 99%

“…It is thought that a p53-dependent postmitotic checkpoint prevents polyploidy. 13 It is however unclear whether wild-type p53 suppresses polyploidy in cells exposed to aurora kinase inhibitors and, importantly, whether normal cells are also susceptible to these drug effects.…”

mentioning

confidence: 99%

Combination of nutlin-3 and VX-680 selectively targets p53 mutant cells with reversible effects on cells expressing wild-type p53

et al. 2010

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Chemotherapeutics (e.g., aurora kinase inhibitors) designed to target proliferative cells are often nonspecific for tumor cells as normal cycling cells are also susceptible. Indeed, one of the major dose-limiting toxicities of aurora kinase inhibitors is a dangerous depletion of neutrophils in patients. In this study we proposed a strategy to selectively target p53 mutant cells while sparing normal ones. The strategy is based on the understanding that normal cells have an intact p53 pathway but not tumor cells carrying p53 mutations. Nongenotoxic activation of p53 using nutlin led to a reversible activation of G1 and G2 arrest in normal cells, which prevents them from entering mitosis, thus protecting them from the side effects of aurora kinase inhibition (VX-680), namely endoreduplication and apoptosis. Cells carrying mutant p53 are selectively killed by the nutlin/VX-680 combination, whereas p53 wild-type cells retain their proliferative capacity. The major implications drawn from these results are:(1) reversible nongenotoxic activation of p53 may be used as a strategy for the chemoprotection of normal tissues, and (2) aurora kinase inhibitors may have alleviated side effects when used in combination with nutlin-like inhibitors. We highlight the distinct roles of p53 and p73 in mediating the cellular responses to VX-680 and suggest that dual protection by p53 and p73 are needed to guard against endoreduplication and polyploidy.

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The Aurora Kinase Inhibitor VX-680 Induces Endoreduplication and Apoptosis Preferentially in Cells with Compromised p53-Dependent Postmitotic Checkpoint Function

Cited by 168 publications

References 34 publications

VX-680 Inhibits Aurora A and Aurora B Kinase Activity in Human Cells

VX-680 Inhibits Aurora A and Aurora B Kinase Activity in Human Cells

Identification of genes that confer tumor cell resistance to the Aurora B kinase inhibitor, AZD1152

Combination of nutlin-3 and VX-680 selectively targets p53 mutant cells with reversible effects on cells expressing wild-type p53

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