EB1 promotes Aurora-B kinase activity through blocking its inactivation by protein phosphatase 2A

Sun, Lei; Gao, Jinmin; Dong, Xin; Liu, Min; Li, Dengwen; Shi, Xingjuan; Dong, Jin‐Tang; Lu, Xiaoyan; Liu, Chunyong; Zhou, Jun

doi:10.1073/pnas.0710018105

Cited by 87 publications

(89 citation statements)

References 26 publications

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“…One of these could be the cyclin-dependent kinase CDKA;1, previously shown to decorate the late PPB and to induce its disassembly [39][40][41][42] , and which co-purified with TON1 in TAP experiments 43 . Aurora kinases, which in animals are functional antagonists of PP2A at the centrosome and microtubule plus ends [44][45][46] , are also putative candidates as suggested by recent results pointing to a function for Aurora kinases in premitotic division plane orientation and cortical cytoskeleton organization 47,48 . Besides a role in PPB formation, the TTP complex likely has a role in interphase cortical array organization as well.…”

Section: Discussionmentioning

confidence: 95%

A protein phosphatase 2A complex spatially controls plant cell division

et al. 2013

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In the absence of cell migration, the orientation of cell divisions is crucial for body plan determination in plants. The position of the division plane in plant cells is set up premitotically via a transient cytoskeletal array, the preprophase band, which precisely delineates the cortical plane of division. Here we describe a protein complex that targets protein phosphatase 2A activity to microtubules, regulating the transition from the interphase to the premitotic microtubule array. This complex, which comprises TONNEAU1 and a PP2A heterotrimeric holoenzyme with FASS as regulatory subunit, is recruited to the cytoskeleton via the TONNEAU1-recruiting motif family of proteins. Despite the acentrosomal nature of plant cells, all members of this complex share similarity with animal centrosomal proteins involved in ciliary and centriolar/centrosomal functions, revealing an evolutionary link between the cortical cytoskeleton of plant cells and microtubule organizers in other eukaryotes.

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Section: Discussionmentioning

confidence: 95%

A protein phosphatase 2A complex spatially controls plant cell division

et al. 2013

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“…The kinase activity of Aurora B is regulated by its phosphorylation level (25,26), and PP2A is a well-known negative regulator of Aurora B (26). Thus, depletion of PPP2R1A may enhance Aurora B activity by increasing its phosphorylation (33,34).…”

Section: Discussionmentioning

confidence: 99%

“…PP2A binds and dephosphorylates Aurora B (25,26). To determine whether Aurora B is involved in the PPP2R1A depletioninduced phenotype, control luciferase siRNA or PPP2R1A siRNA was transfected with or without Aurora B siRNA to HeLa and Mad2-overexpressing HeLa cells, and then a colony formation assay was performed.…”

Section: Aurora B Sirna Decreases Mad2 Phosphorylation In Mitosis Andmentioning

confidence: 99%

Synthetic genetic array screen identifies PP2A as a therapeutic target in Mad2-overexpressing tumors

Bian

Kitagawa

Bansal

et al. 2014

Proc. Natl. Acad. Sci. U.S.A.

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Significance The spindle checkpoint is required for proper chromosome segregation. Mitotic arrest deficiency 2 (Mad2), a component of the spindle checkpoint, is overexpressed in many cancer cells. This phenotype can be used to specifically kill Mad2-overexpressing tumor cells. Because the spindle checkpoint pathway is highly conserved between yeast and humans, we performed a screen to identify mutants in which Mad2 overexpression kills yeast cells. The screen revealed that Mad2 overexpression induced lethality in 13 gene deletions. Among the human homologs of the 13 candidate genes, a gene encoding protein phosphatase 2 (PP2A) significantly inhibited the growth of Mad2-overexpressing tumor cells. These results indicate that PP2A can be a specific therapeutic target in Mad2-overexpressing tumors.

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“…Using Lamin B1 and DAPI staining, we demonstrated that the nuclear envelope was closed and chromosomes were decondensed (Figure 1B); however, in CLL doublet cells the cytoplasm was interconnected (Figure 1A). When we performed immunofluorescence staining for Plk1 and Aurora B, proteins known to regulate cytokinesis,11, 12 we found that Plk1 localized at the cytokinesis contractile ring in CLL doublets (Figure 1C), which is a hallmark of cytokinesis 11. Taken together, our results indicate that CLL cell doublets were in the cytokinesis stage of the cell cycle, specifically, after reformation of the nucleus, but before abscission and physical separation of the cytoplasm 11, 13, 14, 15, 16…”

Section: Resultsmentioning

confidence: 99%

Cytokinesis arrest and multiple centrosomes in B cell chronic lymphocytic leukaemia

Rogne

Svaerd

Madsen‐Østerbye

et al. 2018

J Cellular Molecular Medi

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Cytokinesis failure leads to the emergence of tetraploid cells and multiple centrosomes. Chronic lymphocytic leukaemia (CLL) is the most common haematological malignancy in adults and is characterized by clonal B cell expansion. Here, we show that a significant number of peripheral blood CLL cells are arrested in cytokinesis and that this event occurred after nuclear envelope reformation and before cytoplasmic abscission. mRNA expression data showed that several genes known to be crucial for cell cycle regulation, checkpoint and centromere function, such as ING4, ING5, CDKN1A and CDK4, were significantly dysregulated in CLL samples. Our results demonstrate that CLL cells exhibit difficulties in completing mitosis, which is different from but may, at least in part, explain the previously reported accumulation of CLL cells in G0/1.

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EB1 promotes Aurora-B kinase activity through blocking its inactivation by protein phosphatase 2A

Cited by 87 publications

References 26 publications

A protein phosphatase 2A complex spatially controls plant cell division

A protein phosphatase 2A complex spatially controls plant cell division

Synthetic genetic array screen identifies PP2A as a therapeutic target in Mad2-overexpressing tumors

Cytokinesis arrest and multiple centrosomes in B cell chronic lymphocytic leukaemia

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