Molecular basis of MKLP2-dependent Aurora B transport from chromatin to the anaphase central spindle

The Aurora B chromosomal passenger complex (CPC) is a conserved regulator of mitosis. Its functions require localization first to the chromosome arms and then centromeres in mitosis and subsequently the central spindle in anaphase. Here, we analyze the requirements for core CPC subunits, survivin and INCENP, and the mitotic kinesin-like protein 2 (MKLP2) in targeting to these distinct localizations. Centromere recruitment of the CPC requires interaction of survivin with histone H3 phosphorylated at threonine 3, and we provide a complete structure of this assembly. Furthermore, we show that the INCENP RRKKRR-motif is required for both centromeric localization of the CPC in metaphase and MKLP2-dependent transport in anaphase. MKLP2 and DNA bind competitively to this motif, and INCENP T59 phosphorylation acts as a switch preventing MKLP2 binding in metaphase. In anaphase, CPC binding promotes the microtubule-dependent ATPase activity of MKLP2. These results explain how centromere targeting of the CPC in mitosis is coupled to its movement to the central spindle in anaphase.

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Borealin

The Journal of Cell Biology ◽

10.1083/jcb.200404001 ◽

2004 ◽

Vol 166 (2) ◽

pp. 179-191 ◽

Cited By ~ 275

Author(s):

Reto Gassmann ◽

Ana Carvalho ◽

Alexander J. Henzing ◽

Sandrine Ruchaud ◽

Damien F. Hudson ◽

...

Keyword(s):

Rna Interference ◽

Histone H3 ◽

Aurora B ◽

Mitotic Progression ◽

Aurora B Kinase ◽

Chromosomal Passenger Complex ◽

Central Spindle ◽

Chromosomal Passenger ◽

Bipolar Spindles

The chromosomal passenger complex of Aurora B kinase, INCENP, and Survivin has essential regulatory roles at centromeres and the central spindle in mitosis. Here, we describe Borealin, a novel member of the complex. Approximately half of Aurora B in mitotic cells is complexed with INCENP, Borealin, and Survivin; and Borealin binds Survivin and INCENP in vitro. A second complex contains Aurora B and INCENP, but no Borealin or Survivin. Depletion of Borealin by RNA interference delays mitotic progression and results in kinetochore–spindle misattachments and an increase in bipolar spindles associated with ectopic asters. The extra poles, which apparently form after chromosomes achieve a bipolar orientation, severely disrupt the partitioning of chromosomes in anaphase. Borealin depletion has little effect on histone H3 serine10 phosphorylation. These results implicate the chromosomal passenger holocomplex in the maintenance of spindle integrity and suggest that histone H3 serine10 phosphorylation is performed by an Aurora B–INCENP subcomplex.

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The chromosomal passenger complex controls the function of endosomal sorting complex required for transport-III Snf7 proteins during cytokinesis

Open Biology ◽

10.1098/rsob.120070 ◽

2012 ◽

Vol 2 (5) ◽

pp. 120070 ◽

Cited By ~ 86

Author(s):

Luisa Capalbo ◽

Emilie Montembault ◽

Tetsuya Takeda ◽

Zuni I. Bassi ◽

David M. Glover ◽

...

Keyword(s):

Cell Division ◽

Molecular Basis ◽

Cleavage Site ◽

Human Cells ◽

Membrane Association ◽

Aurora B ◽

Chromosomal Passenger Complex ◽

Endosomal Sorting ◽

Daughter Cells ◽

Chromosomal Passenger

Summary Cytokinesis controls the proper segregation of nuclear and cytoplasmic materials at the end of cell division. The chromosomal passenger complex (CPC) has been proposed to monitor the final separation of the two daughter cells at the end of cytokinesis in order to prevent cell abscission in the presence of DNA at the cleavage site, but the precise molecular basis for this is unclear. Recent studies indicate that abscission could be mediated by the assembly of filaments comprising components of the endosomal sorting complex required for transport-III (ESCRT-III). Here, we show that the CPC subunit Borealin interacts directly with the Snf7 components of ESCRT-III in both Drosophila and human cells. Moreover, we find that the CPC's catalytic subunit, Aurora B kinase, phosphorylates one of the three human Snf7 paralogues—CHMP4C—in its C-terminal tail, a region known to regulate its ability to form polymers and associate with membranes. Phosphorylation at these sites appears essential for CHMP4C function because their mutation leads to cytokinesis defects. We propose that CPC controls abscission timing through inhibition of ESCRT-III Snf7 polymerization and membrane association using two concurrent mechanisms: interaction of its Borealin component with Snf7 proteins and phosphorylation of CHMP4C by Aurora B.

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EB1 enables spindle microtubules to regulate centromeric recruitment of Aurora B

The Journal of Cell Biology ◽

10.1083/jcb.201307119 ◽

2014 ◽

Vol 204 (6) ◽

pp. 947-963 ◽

Cited By ~ 38

Author(s):

Budhaditya Banerjee ◽

Cortney A. Kestner ◽

P. Todd Stukenberg

Keyword(s):

Mitotic Chromosome ◽

Histone H3 ◽

Aurora B ◽

Dependent Manner ◽

Histone H2a ◽

Aurora B Kinase ◽

Chromosomal Passenger Complex ◽

Checkpoint Signaling ◽

Chromosomal Passenger ◽

Spindle Microtubules

The Aurora B kinase coordinates kinetochore–microtubule attachments with spindle checkpoint signaling on each mitotic chromosome. We find that EB1, a microtubule plus end–tracking protein, is required to enrich Aurora B at inner centromeres in a microtubule-dependent manner. This regulates phosphorylation of both kinetochore and chromatin substrates. EB1 regulates the histone phosphorylation marks (histone H2A phospho-Thr120 and histone H3 phospho-Thr3) that localize Aurora B. The chromosomal passenger complex containing Aurora B can be found on a subset of spindle microtubules that exist near prometaphase kinetochores, known as preformed K-fibers (kinetochore fibers). Our data suggest that EB1 enables the spindle microtubules to regulate the phosphorylation of kinetochores through recruitment of the Aurora B kinase.

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Uncoupling the Central Spindle-associated Function of the Chromosomal Passenger Complex from Its Role at Centromeres

Molecular Biology of the Cell ◽

10.1091/mbc.e05-08-0727 ◽

2006 ◽

Vol 17 (4) ◽

pp. 1897-1909 ◽

Cited By ~ 54

Author(s):

Susanne M.A. Lens ◽

Jose A. Rodriguez ◽

Gerben Vader ◽

Simone W. Span ◽

Giuseppe Giaccone ◽

...

Keyword(s):

Spindle Checkpoint ◽

Aurora B ◽

Deletion Mutants ◽

Chromosomal Passenger Complex ◽

Central Spindle ◽

Survivin Protein ◽

C Terminus ◽

Chromosomal Passenger ◽

Associated Function ◽

Bir Domain

Survivin is a component of the chromosomal passenger complex (CPC) that plays a role in maintenance of an active spindle checkpoint and in cytokinesis. To study whether these different functions can be attributed to distinct domains within the Survivin protein, we complemented Survivin-depleted cells with a variety of point- and deletion-mutants of Survivin. We show that an intact baculovirus IAP repeat (BIR) domain is required for proper spindle checkpoint functioning, but dispensable for cytokinesis. In line with this, mutants lacking an intact BIR domain localized normally to the central spindle, but their localization to inner centromeres was severely perturbed. Consequently, these mutants failed to recruit Aurora B, Borealin/Dasra B, and BubR1 to centromeres and kinetochores, but they had retained the ability to recruit Aurora B and Borealin/Dasra B to the midzone and midbody. Thus, the C terminus of Survivin is sufficient for central spindle localization and execution of cytokinesis, but the additional presence of a functional BIR domain is essential for centromere targeting and spindle checkpoint function. Importantly, our data show that the function of the CPC at the centromere can be separated from its function at the central spindle and that execution of cytokinesis does not require prior concentration of the CPC at centromeres.

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Chromosome-directed oocyte spindle assembly depends HP1 and the Chromosomal Passenger Complex

10.1101/2020.06.03.132142 ◽

2020 ◽

Author(s):

Lin-Ing Wang ◽

Tyler DeFosse ◽

Rachel A. Battaglia ◽

Victoria F. Wagner ◽

Kim S. McKim

Keyword(s):

Homologous Chromosome ◽

Spindle Assembly ◽

Aurora B ◽

Aurora B Kinase ◽

Chromosomal Passenger Complex ◽

Central Spindle ◽

Bipolar Spindle ◽

Chromosomal Passenger ◽

Spindle Microtubules

AbstractThe chromosomes in the oocytes of many animals appear to promote bipolar spindle assembly. In Drosophila oocytes, spindle assembly requires the chromosomal passenger complex (CPC), which consists of INCENP, Borealin, Survivin and Aurora B. To determine what recruits the CPC to the chromosomes and its role in spindle assembly, we developed a strategy to manipulate the function and localization of INCENP, which is critical for recruiting the Aurora B kinase. We found that an interaction between Borealin and HP1 is crucial for the initial recruitment of the CPC to the chromosomes and is sufficient to build kinetochores and recruit spindle microtubules. We also found that HP1 moves from the chromosomes to the spindle microtubules along with the CPC, and based on this, propose a mechanism for how the CPC moves from the chromosomes to the microtubules. Within the central spindle, rather than at the centromeres, the CPC and HP1 are required for homologous chromosome bi-orientation.

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Aurora B kinase activity–dependent and –independent functions of the chromosomal passenger complex in regulating sister chromatid cohesion

Journal of Biological Chemistry ◽

10.1074/jbc.ra118.005978 ◽

2018 ◽

Vol 294 (6) ◽

pp. 2021-2035 ◽

Cited By ~ 3

Author(s):

Qi Yi ◽

Qinfu Chen ◽

Haiyan Yan ◽

Miao Zhang ◽

Cai Liang ◽

...

Keyword(s):

Sister Chromatid ◽

Kinase Activity ◽

Sister Chromatid Cohesion ◽

Aurora B ◽

Aurora B Kinase ◽

Chromosomal Passenger Complex ◽

Independent Functions ◽

Chromatid Cohesion ◽

Chromosomal Passenger ◽

Activity Dependent

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Centromere Targeting of the Chromosomal Passenger Complex Requires a Ternary Subcomplex of Borealin, Survivin, and the N-Terminal Domain of INCENP

Molecular Biology of the Cell ◽

10.1091/mbc.e05-12-1133 ◽

2006 ◽

Vol 17 (6) ◽

pp. 2547-2558 ◽

Cited By ~ 104

Author(s):

Ulf R. Klein ◽

Erich A. Nigg ◽

Ulrike Gruneberg

Keyword(s):

Functional Module ◽

Aurora B ◽

Serine Threonine Kinase ◽

Chromosomal Passenger Complex ◽

Chromosomal Passenger ◽

Core Components ◽

Interfering Rna ◽

Centromere Assembly

The chromosomal passenger complex (CPC), consisting of the serine/threonine kinase Aurora B, the inner centromere protein INCENP, Survivin, and Borealin/DasraB, has essential functions at the centromere in ensuring correct chromosome alignment and segregation. Despite observations that small interfering RNA-mediated knockdown of any one member of the CPC abolishes localization of the other subunits, it remains unclear how the complex is targeted to the centromere. We have now identified a ternary subcomplex of the CPC comprising Survivin, Borealin, and the N-terminal 58 amino acids of INCENP in vitro and in vivo. This subcomplex was found to be essential and sufficient for targeting to the centromere. Notably, Aurora B kinase, the enzymatic core of the CPC, was not required for centromere localization of the subcomplex. We demonstrate that CPC targeting to the centromere does not depend on CENP-A and hMis12, two core components for kinetochore/centromere assembly, and provide evidence that the CPC may be directed to centromeric DNA directly via the Borealin subunit. Our findings thus establish a functional module within the CPC that assembles on the N terminus of INCENP and controls centromere recruitment.

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Molecular Basis for CPC-Sgo1 Interaction: Implications for Centromere Localisation and Function of the CPC

10.1101/2021.08.27.457910 ◽

2021 ◽

Author(s):

Maria Alba Abad ◽

Tanmay Gupta ◽

Michael A Hadders ◽

Amanda Meppelink ◽

J Pepijn Wopken ◽

...

Keyword(s):

Chromosome Segregation ◽

Molecular Basis ◽

Hot Spot ◽

Histone H3 ◽

Direct Interaction ◽

Histone H2a ◽

Chromosomal Passenger ◽

And Function ◽

Affinity Interaction

AbstractThe Chromosomal Passenger Complex (CPC; consisting of Borealin, Survivin, INCENP and Aurora B kinase) and Shugoshin 1 (Sgo1) are key regulators of chromosome bi-orientation, a process essential for error-free chromosome segregation. Their functions rely on their ability to associate with centromeres. Two histone phosphorylations, histone H3 Thr3 (H3T3ph; directly recognised by Survivin) and histone H2A Thr120 (H2AT120ph; indirectly recognised via Sgo1), together with CPC’s intrinsic ability to bind nucleosome, facilitate CPC centromere recruitment. The molecular basis for CPC-Sgo1 binding and how their direct interaction influences CPC centromere localisation and function are lacking. Here, using an integrative structure-function approach, we show that the histone H3-like Sgo1 N-terminal tail interacts with Survivin acting as a hot-spot for CPC-Sgo1 assembly, while downstream Sgo1 residues, mainly with Borealin contributes for high affinity interaction. Disruption of the Sgo1 N-terminal tail-Survivin interaction abolished CPC-Sgo1 assembly in vitro and perturbed centromere localisation and function of CPC. Our findings provide evidence that CPC binding to Sgo1 and histone H3 N-terminal tail are mutually exclusive, suggesting that these interactions will likely take place in a spatially/temporally restricted manner and provide a rationale for the Sgo1-mediated ‘kinetochore proximal centromere’ pool of CPC.

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Borealin–nucleosome interaction secures chromosome association of the chromosomal passenger complex

The Journal of Cell Biology ◽

10.1083/jcb.201905040 ◽

2019 ◽

Vol 218 (12) ◽

pp. 3912-3925 ◽

Cited By ~ 7

Author(s):

Maria A. Abad ◽

Jan G. Ruppert ◽

Lana Buzuk ◽

Martin Wear ◽

Juan Zou ◽

...

Keyword(s):

Cell Division ◽

Chromosome Segregation ◽

Chromosome Association ◽

Aurora B ◽

Master Regulator ◽

Multifaceted Approach ◽

Chromosomal Passenger Complex ◽

Chromosome Congression ◽

Chromosomal Passenger ◽

And Function

Chromosome association of the chromosomal passenger complex (CPC; consisting of Borealin, Survivin, INCENP, and the Aurora B kinase) is essential to achieve error-free chromosome segregation during cell division. Hence, understanding the mechanisms driving the chromosome association of the CPC is of paramount importance. Here using a multifaceted approach, we show that the CPC binds nucleosomes through a multivalent interaction predominantly involving Borealin. Strikingly, Survivin, previously suggested to target the CPC to centromeres, failed to bind nucleosomes on its own and requires Borealin and INCENP for its binding. Disrupting Borealin–nucleosome interactions excluded the CPC from chromosomes and caused chromosome congression defects. We also show that Borealin-mediated chromosome association of the CPC is critical for Haspin- and Bub1-mediated centromere enrichment of the CPC and works upstream of the latter. Our work thus establishes Borealin as a master regulator determining the chromosome association and function of the CPC.

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The Borealin dimerization domain interacts with Sgo1 to drive Aurora B–mediated spindle assembly

Molecular Biology of the Cell ◽

10.1091/mbc.e20-05-0341 ◽

2020 ◽

Vol 31 (20) ◽

pp. 2207-2218 ◽

Cited By ~ 1

Author(s):

Mary Kate Bonner ◽

Julian Haase ◽

Hayden Saunders ◽

Hindol Gupta ◽

Biyun Iris Li ◽

...

Keyword(s):

Molecular Mechanism ◽

Spindle Assembly ◽

Specific Role ◽

Aurora B ◽

Dimerization Domain ◽

Chromosomal Passenger Complex ◽

Chromosomal Passenger ◽

Segregation Of Chromosomes

This study provides the molecular mechanism for the interaction of Sgo1 with the chromosomal passenger complex and explores the specific role of Sgo1 in regulating Aurora B functions that ensure the equal segregation of chromosomes.

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