50 ways to build a spindle: the complexity of microtubule generation during mitosis

Duncan, Tommy; Wakefield, James G.

doi:10.1007/s10577-011-9205-8

Cited by 35 publications

(31 citation statements)

References 102 publications

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“…Although centrosome-derived microtubules are radial initially, they begin growing with directional bias so that the density of microtubules between centrosomes and the mitotic chromosomes is greater than between centrosomes and the cell cortex (42). These observations suggest a lack of equality in the extension of microtubules to the cortex or to chromosomes.…”

Section: Discussionmentioning

confidence: 94%

“…These observations suggest a lack of equality in the extension of microtubules to the cortex or to chromosomes. It remains unclear what elements, including microtubule-associated proteins or motor proteins, cause this directional activity (42). HURP is one element that participates in this asymmetry through its association with microtubules that grow toward the mitotic chromosomes rather than the cortex (Fig.…”

Section: Discussionmentioning

confidence: 99%

See 1 more Smart Citation

Aurora kinase inhibitors reveal mechanisms of HURP in nucleation of centrosomal and kinetochore microtubules

Wu¹,

Chen²,

Coumar

et al. 2013

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

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The overexpression of Aurora kinases in multiple tumors makes these kinases appealing targets for the development of anticancer therapies. This study identified two small molecules with a furanopyrimidine core, IBPR001 and IBPR002, that target Aurora kinases and induce a DFG conformation change at the ATP site of Aurora A. Our results demonstrate the high potency of the IBPR compounds in reducing tumorigenesis in a colorectal cancer xenograft model in athymic nude mice. Human hepatoma up-regulated protein (HURP) is a substrate of Aurora kinase A, which plays a crucial role in the stabilization of kinetochore fibers. This study used the IBPR compounds as well as MLN8237, a proven Aurora A inhibitor, as chemical probes to investigate the molecular role of HURP in mitotic spindle formation. These compounds effectively eliminated HURP phosphorylation, thereby revealing the coexistence and continuous cycling of HURP between unphosphorylated and phosphorylated forms that are associated, respectively, with microtubules emanating from centrosomes and kinetochores. Furthermore, these compounds demonstrate a spatial hierarchical preference for HURP in the attachment of microtubules extending from the mother to the daughter centrosome. The finding of inequality in the centrosomal microtubules revealed by these small molecules provides a versatile tool for the discovery of new cell-division molecules for the development of antitumor drugs.

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Section: Discussionmentioning

confidence: 94%

Section: Discussionmentioning

confidence: 99%

Aurora kinase inhibitors reveal mechanisms of HURP in nucleation of centrosomal and kinetochore microtubules

Wu¹,

Chen²,

Coumar

et al. 2013

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

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“…This raises a possibility that the augmin complex may contain more than one MAP. Structurally, Msd1/ Dgt9 and HAUS2/Cep27 can be paired with each other (Duncan and Wakefield, 2011). Because of its sequence similarity to HAUS2, it would be interesting to test whether AUG2 also interacts with MTs directly.…”

Section: The Arabidopsis Augmin Complex Contains Both Conserved and Umentioning

confidence: 99%

“…Multiple mechanisms are known to contribute to the assembly of the spindle apparatus in animal cells (Duncan and Wakefield, 2011). Whereas some are dependent on the g-tubulin complex, others rely on proteins like the Ran GTPase and MAP/ motors.…”

Section: Augmin-dependent Spindle Morphogenesis In Plant Cellsmentioning

confidence: 99%

Characterization of the Arabidopsis Augmin Complex Uncovers Its Critical Function in the Assembly of the Acentrosomal Spindle and Phragmoplast Microtubule Arrays

et al. 2012

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Plant cells assemble the bipolar spindle and phragmoplast microtubule (MT) arrays in the absence of the centrosome structure. Our recent findings in Arabidopsis thaliana indicated that AUGMIN subunit3 (AUG3), a homolog of animal dim gtubulin 3, plays a critical role in g-tubulin-dependent MT nucleation and amplification during mitosis. Here, we report the isolation of the entire plant augmin complex that contains eight subunits. Among them, AUG1 to AUG6 share low sequence similarity with their animal counterparts, but AUG7 and AUG8 share homology only with proteins of plant origin. Genetic analyses indicate that the AUG1, AUG2, AUG4, and AUG5 genes are essential, as stable mutations in these genes could only be transmitted to heterozygous plants. The sterile aug7-1 homozygous mutant in which AUG7 expression is significantly reduced exhibited pleiotropic phenotypes of seriously retarded vegetative and reproductive growth. The aug7-1 mutation caused delocalization of g-tubulin in the mitotic spindle and phragmoplast. Consequently, spindles were abnormally elongated, and their poles failed to converge, as MTs were splayed to discrete positions rendering deformed arrays. In addition, the mutant phragmoplasts often had disorganized MT bundles with uneven edges. We conclude that assembly of MT arrays during plant mitosis depends on the augmin complex, which includes two plant-specific subunits.

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“…However, recent reports from Drosophila indicate that spindle assembly pathways vary between the two dividing cell types. 34,[46][47][48] Therefore, it remains to be determined whether the plus and minus end effectors are shared or whether spermatocytes use alternative depolymerization mechanisms. Elucidating the molecules involved is an exciting future challenge that will require the application of the photobleaching assay to cells manipulated by genetic or pharmacological methods.…”

Section: Savoian / Photobleaching Spermatocyte Microtubulesmentioning

confidence: 99%

Using Photobleaching to Measure Spindle Microtubule Dynamics in Primary Cultures of Dividing Drosophila Meiotic Spermatocytes

Savoian

2015

J Biomol Tech

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In dividing animal cells, a microtubule (MT)-based bipolar spindle governs chromosome movement. Current models propose that the spindle facilitates and/or generates translocating forces by regionally depolymerizing the kinetochore fibers (k-fibers) that bind each chromosome. It is unclear how conserved these sites and the resultant chromosome-moving mechanisms are between different dividing cell types because of the technical challenges of quantitatively studying MTs in many specimens. In particular, our knowledge of MT kinetics during the sperm-producing male meiotic divisions remains in its infancy. In this study, I use an easy-to-implement photobleaching-based assay for measuring spindle MT dynamics in primary cultures of meiotic spermatocytes isolated from the fruit fly Drosophila melanogaster. By use of standard scanning confocal microscopy features, fiducial marks were photobleached on fluorescent protein (FP)-tagged MTs. These were followed by time-lapse imaging during different division stages, and their displacement rates were calculated using public domain software. I find that k-fibers continually shorten at their poles during metaphase and anaphase A through the process of MT flux. Anaphase chromosome movement is complemented by Pac-Man, the shortening of the k-fiber at its chromosomal interface. Thus, Drosophila spermatocytes share the sites of spindle dynamism and mechanisms of chromosome movement with mitotic cells. The data reveal the applicability of the photobleaching assay for measuring MT dynamics in primary cultures. This approach can be readily applied to other systems.

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50 ways to build a spindle: the complexity of microtubule generation during mitosis

Cited by 35 publications

References 102 publications

Aurora kinase inhibitors reveal mechanisms of HURP in nucleation of centrosomal and kinetochore microtubules

Aurora kinase inhibitors reveal mechanisms of HURP in nucleation of centrosomal and kinetochore microtubules

Characterization of the Arabidopsis Augmin Complex Uncovers Its Critical Function in the Assembly of the Acentrosomal Spindle and Phragmoplast Microtubule Arrays

Using Photobleaching to Measure Spindle Microtubule Dynamics in Primary Cultures of Dividing Drosophila Meiotic Spermatocytes

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