Late mitotic functions of Aurora kinases

Afonso, Olga; Figueiredo, Ana C.; Maiato, Hélder

doi:10.1007/s00412-016-0594-5

Cited by 45 publications

(44 citation statements)

References 122 publications

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“…AURKA activity increases in preparation for mitosis in parallel with the protein level, and both progressively drop from anaphase onwards. This has led to the expectation that destruction contributes to regulating AURKA activity at mitotic exit [28,33]. We observed, however, that loss of AURKA activity proceeds faster than destruction of the protein.…”

Section: Discussionmentioning

confidence: 71%

“…Although AURKA activity has been described to peak in M phase there has been no detailed characterization of how AURKA activity varies through mitosis. In particular the question of how AURKA activity is regulated during mitotic exit, given that AURKA also has anaphase functions [32,33], and the importance of its ongoing destruction for attenuation of activity, remain unresolved. We first used a commercially available antibody against the activated T-loop of Aurora kinases (pT288 in AURKA) that confirms by immunoblot the peak of active AURKA at mitosis in extracts from synchronised U2OS cells ( Figure 1A).…”

Section: Resultsmentioning

confidence: 99%

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AURKA destruction is decoupled from its activity at mitotic exit but suppresses interphase activity

Abdelbaki

Akman

Poteau³

et al. 2019

Preprint

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Activity of AURKA is controlled through multiple mechanisms including phosphorylation, ubiquitinmediated degradation, and allosteric interaction with TPX2. Activity peaks at mitosis before AURKA is degraded during mitotic exit in a process strictly dependent on APC/C coactivator FZR1. We used FZR1 knockout cells (FZR1 KO ) and a novel FRET-based AURKA biosensor to investigate how activity is regulated in absence of destruction. We found that AURKA activity in FZR1 KO cells dropped at mitotic exit as rapidly as in parental cells, despite absence of destruction. Unexpectedly, TPX2 was degraded normally in FZR1 KO cells. Overexpression of an N-terminal TPX2 fragment sufficient for AURKA binding, but not degraded at mitotic exit, caused delay in AURKA inactivation. We conclude that AURKA inactivation in mitotic exit is determined not by its own degradation but by degradation of TPX2 and therefore dependent on CDC20 rather than FZR1. The biosensor revealed that FZR1 instead suppresses AURKA activity in interphase and is critically required for assembly of the interphase mitochondrial network after mitosis.

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Section: Discussionmentioning

confidence: 71%

Section: Resultsmentioning

confidence: 99%

AURKA destruction is decoupled from its activity at mitotic exit but suppresses interphase activity

Abdelbaki

Akman

Poteau³

et al. 2019

Preprint

View full text Add to dashboard Cite

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“…It is also required for correct chromosome alignment and segregation during metaphase, and therefore regulates kinetochore functions (Afonso et al., 2016, Cheng et al., 2011, Lampson and Cheeseman, 2011). In addition, Aurora B plays critical roles in spindle checkpoint and cytokinesis (Ruchaud et al., 2007, Steigemann et al., 2008).…”

Section: Resultsmentioning

confidence: 99%

Single-Cell Dynamic Analysis of Mitosis in Haploid Embryonic Stem Cells Shows the Prolonged Metaphase and Its Association with Self-diploidization

Guo

Huang

et al. 2017

Stem Cell Reports

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SummaryThe recent establishment of mammalian haploid embryonic stem cells (ESCs) provides new possibilities for genetic screening and for understanding genome evolution and function. However, the dynamics of mitosis in haploid ESCs is still unclear. Here, we report that the duration of mitosis in haploid ESCs, especially the metaphase, is significantly longer than that in diploid ESCs. Delaying mitosis by chemicals increased self-diploidization of haploid ESCs, while shortening mitosis stabilized haploid ESCs. Taken together, our study suggests that the delayed mitosis of haploid ESCs is associated with self-diploidization.

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“…The budding yeast Polo-like kinase Cdc5 is essential for mitotic entry, chromosome segregation, and cytokinesis (Botchkarev & Haber, 2017). The Aurora kinase Ipl1 in turn is an integral part of the mitotic chromosome biorientation and segregation mechanism, with additional functions in the control of cytokinesis in higher eukaryotes (Afonso et al, 2017). Polo and Aurora kinases recognize (D/E/N)x (S/T) and (K/R)(K/R)x(S/T) motifs, respectively (Mok et al, 2010;Alexander et al, 2011).…”

Section: Introductionmentioning

confidence: 99%

Phosphoproteome dynamics during mitotic exit in budding yeast

et al. 2018

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The cell division cycle culminates in mitosis when two daughter cells are born. As cyclin‐dependent kinase (Cdk) activity reaches its peak, the anaphase‐promoting complex/cyclosome (APC/C) is activated to trigger sister chromatid separation and mitotic spindle elongation, followed by spindle disassembly and cytokinesis. Degradation of mitotic cyclins and activation of Cdk‐counteracting phosphatases are thought to cause protein dephosphorylation to control these sequential events. Here, we use budding yeast to analyze phosphorylation dynamics of 3,456 phosphosites on 1,101 proteins with high temporal resolution as cells progress synchronously through mitosis. This reveals that successive inactivation of S and M phase Cdks and of the mitotic kinase Polo contributes to order these dephosphorylation events. Unexpectedly, we detect as many new phosphorylation events as there are dephosphorylation events. These correlate with late mitotic kinase activation and identify numerous candidate targets of these kinases. These findings revise our view of mitotic exit and portray it as a dynamic process in which a range of mitotic kinases contribute to order both protein dephosphorylation and phosphorylation.

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Late mitotic functions of Aurora kinases

Cited by 45 publications

References 122 publications

AURKA destruction is decoupled from its activity at mitotic exit but suppresses interphase activity

AURKA destruction is decoupled from its activity at mitotic exit but suppresses interphase activity

Single-Cell Dynamic Analysis of Mitosis in Haploid Embryonic Stem Cells Shows the Prolonged Metaphase and Its Association with Self-diploidization

Phosphoproteome dynamics during mitotic exit in budding yeast

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