Exploring the Functional Interactions between Aurora B, INCENP, and Survivin in Mitosis

Honda, Reiko; Körner, Roman; Nigg, Erich A.

doi:10.1091/mbc.e02-11-0769

Cited by 476 publications

(583 citation statements)

References 58 publications

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“…Aurora B undergoes CRM1-mediated nuclear export The nucleocytoplasmic distribution of Aurora B fused to a MYC tag, similar in size to the VSV and HA epitopes used here, has been previously shown to be predominantly nuclear in U2OS cells (Honda et al, 2003), and both nuclear and cytoplasmic in COS-7 cells (Kawajiri et al, 2003;Yasui et al, 2004). These previous observations, and the heterogeneous distribution we found in MCF-7 cells, suggested that the nucleocytoplasmic distribution of Aurora B before NEB could be a dynamic process.…”

Section: Resultssupporting

confidence: 80%

“…INCENP is a large protein that has been proposed to act as a scaffold for the binding of the other passenger proteins (Bolton et al, 2002). Aurora B phosphorylates INCENP, which, in turn, activates the kinase activity of Aurora B in a positive feedback loop (Bishop and Schumacher, 2002;Honda et al, 2003). Survivin is a member of the inhibitor of apoptosis protein family that plays a dual role as regulator of both apoptosis and cell division (reviewed by Altieri, 2003a).…”

Section: Introductionmentioning

confidence: 99%

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Subcellular localization and nucleocytoplasmic transport of the chromosomal passenger proteins before nuclear envelope breakdown

et al. 2006

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As mitosis progresses, the chromosomal passenger proteins (CPPs) Survivin, Aurora B, INCENP and Borealin dynamically colocalize to mitotic structures. Chromosomal passenger proteins are already expressed during G2, whereas the nuclear envelope is only disassembled at the end of prophase. However, the mechanisms that modulate their nucleocytoplasmic localization before nuclear envelope breakdown (NEB) are poorly characterized. Using epitope-tagged proteins, we show that Aurora B, like Survivin, undergoes CRM1-mediated nucleocytoplasmic shuttling, although both proteins lack identifiable 'classical' nuclear transport signals. On the other hand, INCENP resides more stably in the nucleus and contains multiple nuclear localization signals. Finally, Borealin was detected in the nucleolus and the cytoplasm, but its cytoplasmic localization is not directly regulated by CRM1. Coexpression experiments indicate that the nuclear localization of Aurora B, but not of Survivin, is modulated by INCENP and that Survivin prevents the nucleolar accumulation of Borealin. Our data reveal that, in contrast to their closely related localization during mitosis, the nucleocytoplasmic localization of the CPPs before NEB is largely unrelated. Furthermore, the specific effect of INCENP and Survivin on the localization of Aurora B and Borealin, respectively, suggests that different complexes of CPPs may exist not only during mitosis, as recently reported, but also before NEB.

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Section: Resultssupporting

confidence: 80%

Section: Introductionmentioning

confidence: 99%

Subcellular localization and nucleocytoplasmic transport of the chromosomal passenger proteins before nuclear envelope breakdown

et al. 2006

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“…Three members of the passenger complex are: INCENP, Aurora B kinase and survivin. INCENP, a microtubule-binding protein is responsible for binding Aurora B (Honda et al, 2003). Survivin has an essential role in chromosome alignment (Lens et al, 2003) and is important during mitosis for proper localization of INCENP and Aurora B (reviewed by Carmena and Earnshaw, 2003).…”

Section: Introductionmentioning

confidence: 99%

Chromosomes with delayed replication timing lead to checkpoint activation, delayed recruitment of Aurora B and chromosome instability

et al. 2006

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Certain chromosome rearrangements display a significant delay in chromosome replication timing (DRT) that is associated with a subsequent delay in mitotic chromosome condensation (DMC). DRT/DMC chromosomes are common in tumor cells in vitro and in vivo and occur frequently in cells exposed to ionizing radiation. A hallmark for these chromosomes is the delayed phosphorylation of serine 10 of histone H3 during mitosis. The chromosome passenger complex, consisting of multiple proteins including Aurora B kinase and INCENP is thought to be responsible for H3 phosphorylation, chromosome condensation and the subsequent segregation of chromosomes. In this report, we show that chromosomes with DRT/DMC contain phosphorylated Chk1, consistent with activation of the S-M phase checkpoint. Furthermore, we show that INCENP is recruited to the DRT/DMC chromosomes during all phases of mitosis. In contrast, Aurora B kinase is absent on DRT/DMC chromosomes when these chromosomes lack serine 10 phosphorylation of H3. We also show that mitotic arrest deficient 2 (Mad2), a member of the spindle assembly checkpoint, is present on DRT/DMC chromosomes at a time when the normally condensed chromosomes show no Mad2 staining, indicating that DRT/DMC activates the spindle assembly checkpoint. Finally, cells with DRT/ DMC chromosomes have centrosome amplification, abnormal spindle assembly, endoreduplication and significant chromosome instability.

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“…Since Survivin has both nuclear and cytoplasmic targets, which appear to serve different functions (Mahotka et al, 2002), two different commercially available Survivin antibodies, which recognise predominantly nuclear and cytoplasmic forms of Survivin, were used (Altura et al, 2003). Nuclear Survivin has been suggested to play an important role in chromosomal segregation during mitosis Honda et al, 2003), while cytoplasmic Survivin has been characterised as antiapoptotic (O'Connor et al, 2002). In addition, the TUNEL assay was used to detect the apoptotic status of the GBMs and apoptotic status was correlated with the expression of different Survivin forms.…”

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confidence: 99%

Expression of cytoplasmic and nuclear Survivin in primary and secondary human glioblastoma

et al. 2005

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Clinically, human glioblastoma (GBM) may develop de novo or from a low-grade glioma (secondary GBM), and molecular alterations in the two pathways may differ. This study examined the status of Survivin expression and apoptosis in 30 primary and 26 secondary GBMs. Our results show that cytoplasmic Survivin positivity was significantly (Po0.001) more frequent in primary GBMs (83%) than that in secondary GBMs (46%). In addition, an inverse correlation of cytoplasmc Survivin positivity with GBM apoptotic index, and a positive association between cytoplasmic Survivin and size of the tumours were observed. These results suggest that cytoplasmic Survivin, via its antiapoptotic function, may be involved in the tumorigenesis of many primary GBMs, but only in a small fraction of secondary GBMs. Furthermore, the overall progression times from low-grade precursor lesions to secondary GBMs were significantly shorter (Po0.05) in cytoplasmic Survivin-positive cases (mean, 15.6 months) than those in Survivin-negative cases (mean, 23.8 moths), and the positive expression level of Survivin in cytoplasm was upregulated in most secondary GBMs when compared to matched pre-existing low-graded lesions. These results suggest that the increased accumulation of Survivin in the cytoplasm of more malignant glioma cells may prove to be a selective advantage, thus accelerating progression to a more aggressive phenotype.

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Exploring the Functional Interactions between Aurora B, INCENP, and Survivin in Mitosis

Cited by 476 publications

References 58 publications

Subcellular localization and nucleocytoplasmic transport of the chromosomal passenger proteins before nuclear envelope breakdown

Subcellular localization and nucleocytoplasmic transport of the chromosomal passenger proteins before nuclear envelope breakdown

Chromosomes with delayed replication timing lead to checkpoint activation, delayed recruitment of Aurora B and chromosome instability

Expression of cytoplasmic and nuclear Survivin in primary and secondary human glioblastoma

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