A mammalian partner of inscuteable binds NuMA and regulates mitotic spindle organization

Quansheng Du; P. Todd Stukenberg; Ian G. Macara

doi:10.1038/ncb1201-1069

A mammalian partner of inscuteable binds NuMA and regulates mitotic spindle organization

Quansheng Du, P. Todd Stukenberg, Ian G. Macara

Research output: Contribution to journal › Article › peer-review

227 Scopus citations

Abstract

Asymmetric cell division requires the orientation of mitotic spindles along the cell-polarity axis. In Drosophila neuroblasts, this involves the interaction of the proteins Inscuteable (Insc) and Partner of inscuteable (Pins). We report here that a human Pins-related protein, called LGN, is instead essential for the assembly and organization of the mitotic spindle. LGN is cytoplasmic in interphase cells, but associates with the spindle poles during mitosis. Ectopic expression of LGN disrupts spindle-pole organization and chromosome segregation. Silencing of LGN expression by RNA interference also disrupts spindle-pole organization and prevents normal chromosome segregation. We found that LGN binds the nuclear mitotic apparatus protein NuMA, which tethers spindles at the poles, and that this interaction is required for the LGN phenotype. Anti-LGN antibodies and the LGN-binding domain of NuMA both trigger microtubule aster formation in mitotic Xenopus egg extracts, and the NuMA-binding domain of LGN blocks aster assembly in egg extracts treated with taxol. Thus, we have identified a mammalian Pins homologue as a key regulator of spindle organization during mitosis.

Original language	English (US)
Pages (from-to)	1069-1075
Number of pages	7
Journal	Nature Cell Biology
Volume	3
Issue number	12
DOIs	https://doi.org/10.1038/ncb1201-1069
State	Published - 2001
Externally published	Yes

ASJC Scopus subject areas

Cell Biology

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title = "A mammalian partner of inscuteable binds NuMA and regulates mitotic spindle organization",

abstract = "Asymmetric cell division requires the orientation of mitotic spindles along the cell-polarity axis. In Drosophila neuroblasts, this involves the interaction of the proteins Inscuteable (Insc) and Partner of inscuteable (Pins). We report here that a human Pins-related protein, called LGN, is instead essential for the assembly and organization of the mitotic spindle. LGN is cytoplasmic in interphase cells, but associates with the spindle poles during mitosis. Ectopic expression of LGN disrupts spindle-pole organization and chromosome segregation. Silencing of LGN expression by RNA interference also disrupts spindle-pole organization and prevents normal chromosome segregation. We found that LGN binds the nuclear mitotic apparatus protein NuMA, which tethers spindles at the poles, and that this interaction is required for the LGN phenotype. Anti-LGN antibodies and the LGN-binding domain of NuMA both trigger microtubule aster formation in mitotic Xenopus egg extracts, and the NuMA-binding domain of LGN blocks aster assembly in egg extracts treated with taxol. Thus, we have identified a mammalian Pins homologue as a key regulator of spindle organization during mitosis.",

author = "Quansheng Du and Stukenberg, {P. Todd} and Macara, {Ian G.}",

note = "Funding Information: ACKNOWLEDGEMENTS We thank G. Post (University of Kentucky) for the human LGN cDNA, J. Casanova (University of Virginia) for the MDCK T23 cell line, Duane Compton (Dartmouth Medical School) for anti-NuMA antibodies and NuMA cDNA, and members of the Macara group for reagents and helpful discussions. We also thank T. Tuschl for information on designing and using siRNA duplexes. This work was supported by grant CA40042 from the NIH, DHHS. Correspondence and requests for materials should be addressed to Q.D. Supplementary Information is available at Nature Cell Biology{\textquoteright}s website (http://nature.cellbio.com).",

year = "2001",

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N1 - Funding Information: ACKNOWLEDGEMENTS We thank G. Post (University of Kentucky) for the human LGN cDNA, J. Casanova (University of Virginia) for the MDCK T23 cell line, Duane Compton (Dartmouth Medical School) for anti-NuMA antibodies and NuMA cDNA, and members of the Macara group for reagents and helpful discussions. We also thank T. Tuschl for information on designing and using siRNA duplexes. This work was supported by grant CA40042 from the NIH, DHHS. Correspondence and requests for materials should be addressed to Q.D. Supplementary Information is available at Nature Cell Biology’s website (http://nature.cellbio.com).

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N2 - Asymmetric cell division requires the orientation of mitotic spindles along the cell-polarity axis. In Drosophila neuroblasts, this involves the interaction of the proteins Inscuteable (Insc) and Partner of inscuteable (Pins). We report here that a human Pins-related protein, called LGN, is instead essential for the assembly and organization of the mitotic spindle. LGN is cytoplasmic in interphase cells, but associates with the spindle poles during mitosis. Ectopic expression of LGN disrupts spindle-pole organization and chromosome segregation. Silencing of LGN expression by RNA interference also disrupts spindle-pole organization and prevents normal chromosome segregation. We found that LGN binds the nuclear mitotic apparatus protein NuMA, which tethers spindles at the poles, and that this interaction is required for the LGN phenotype. Anti-LGN antibodies and the LGN-binding domain of NuMA both trigger microtubule aster formation in mitotic Xenopus egg extracts, and the NuMA-binding domain of LGN blocks aster assembly in egg extracts treated with taxol. Thus, we have identified a mammalian Pins homologue as a key regulator of spindle organization during mitosis.

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A mammalian partner of inscuteable binds NuMA and regulates mitotic spindle organization

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