KIFC3 promotes mitotic progression and integrity of the central spindle in cytokinesis

Jeannette Nachbar; Francisco Laźaro-Diéguez; Rytis Prekeris; David Cohen; Anne Mus̈ch

doi:10.4161/cc.27266

KIFC3 promotes mitotic progression and integrity of the central spindle in cytokinesis

Jeannette Nachbar, Francisco Laźaro-Diéguez, Rytis Prekeris, David Cohen, Anne Mus̈ch

Developmental & Molecular Biology

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

6 Scopus citations

Abstract

Kinesin-14 motor proteins play a variety of roles during metaphase and anaphase. However, it is not known whether members of this family of motors also participate in the dramatic changes in mitotic spindle organization during the transition from telophase to cytokinesis. We have identified the minus-end-directed motor, KIFC3, as an important contributor to central bridge morphology at this stage. KIFC3's unique motor-dependent localization at the central bridge allows it to congress microtubules, promoting efficient progress through cytokinesis. Conversely, when KIFC3 function is perturbed, abscission is delayed, and the central bridge is both widened and extended. Examination of KIFC3 on growing microtubules in interphase indicates that it caps microtubules released from the centrosome, both in the region of the centrosome and in the cell periphery. In line with other kinesin-14 family members, KIFC3 may guide free microtubules to their destination at the bridge and/or may slide and crosslink central bridge microtubules in order to stage the cells for abscission.

Original language	English (US)
Pages (from-to)	426-433
Number of pages	8
Journal	Cell Cycle
Volume	13
Issue number	3
DOIs	https://doi.org/10.4161/cc.27266
State	Published - Feb 1 2014

Keywords

Abscission
Cytokinesis
KIFC3
Kinesin-14
Mitotic kinesin

ASJC Scopus subject areas

Molecular Biology
Developmental Biology
Cell Biology

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title = "KIFC3 promotes mitotic progression and integrity of the central spindle in cytokinesis",

abstract = "Kinesin-14 motor proteins play a variety of roles during metaphase and anaphase. However, it is not known whether members of this family of motors also participate in the dramatic changes in mitotic spindle organization during the transition from telophase to cytokinesis. We have identified the minus-end-directed motor, KIFC3, as an important contributor to central bridge morphology at this stage. KIFC3's unique motor-dependent localization at the central bridge allows it to congress microtubules, promoting efficient progress through cytokinesis. Conversely, when KIFC3 function is perturbed, abscission is delayed, and the central bridge is both widened and extended. Examination of KIFC3 on growing microtubules in interphase indicates that it caps microtubules released from the centrosome, both in the region of the centrosome and in the cell periphery. In line with other kinesin-14 family members, KIFC3 may guide free microtubules to their destination at the bridge and/or may slide and crosslink central bridge microtubules in order to stage the cells for abscission.",

keywords = "Abscission, Cytokinesis, KIFC3, Kinesin-14, Mitotic kinesin",

author = "Jeannette Nachbar and Francisco La{\'z}aro-Di{\'e}guez and Rytis Prekeris and David Cohen and Anne Mu{\"s}ch",

note = "Funding Information: We thank Drs Lawrence Goldstein and Chloe Bulinski for providing cDNAs and we are grateful to Dr Ching-Hwa Sung for making her EB1-GFP-MDCK cell available to us and to Dr Thomas Weimbs for the MDCK TET-ON cells. This work was supported by NIH/NIDDK R01KD064842-07A1 and NIH/ NCI 1R01CA1607901-01 to AM and by funds from the Sue Golding Graduate Program at the Albert-Einstein College of Medicine to JN.",

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AU - Nachbar, Jeannette

AU - Laźaro-Diéguez, Francisco

AU - Prekeris, Rytis

AU - Cohen, David

AU - Mus̈ch, Anne

N1 - Funding Information: We thank Drs Lawrence Goldstein and Chloe Bulinski for providing cDNAs and we are grateful to Dr Ching-Hwa Sung for making her EB1-GFP-MDCK cell available to us and to Dr Thomas Weimbs for the MDCK TET-ON cells. This work was supported by NIH/NIDDK R01KD064842-07A1 and NIH/ NCI 1R01CA1607901-01 to AM and by funds from the Sue Golding Graduate Program at the Albert-Einstein College of Medicine to JN.

PY - 2014/2/1

Y1 - 2014/2/1

N2 - Kinesin-14 motor proteins play a variety of roles during metaphase and anaphase. However, it is not known whether members of this family of motors also participate in the dramatic changes in mitotic spindle organization during the transition from telophase to cytokinesis. We have identified the minus-end-directed motor, KIFC3, as an important contributor to central bridge morphology at this stage. KIFC3's unique motor-dependent localization at the central bridge allows it to congress microtubules, promoting efficient progress through cytokinesis. Conversely, when KIFC3 function is perturbed, abscission is delayed, and the central bridge is both widened and extended. Examination of KIFC3 on growing microtubules in interphase indicates that it caps microtubules released from the centrosome, both in the region of the centrosome and in the cell periphery. In line with other kinesin-14 family members, KIFC3 may guide free microtubules to their destination at the bridge and/or may slide and crosslink central bridge microtubules in order to stage the cells for abscission.

AB - Kinesin-14 motor proteins play a variety of roles during metaphase and anaphase. However, it is not known whether members of this family of motors also participate in the dramatic changes in mitotic spindle organization during the transition from telophase to cytokinesis. We have identified the minus-end-directed motor, KIFC3, as an important contributor to central bridge morphology at this stage. KIFC3's unique motor-dependent localization at the central bridge allows it to congress microtubules, promoting efficient progress through cytokinesis. Conversely, when KIFC3 function is perturbed, abscission is delayed, and the central bridge is both widened and extended. Examination of KIFC3 on growing microtubules in interphase indicates that it caps microtubules released from the centrosome, both in the region of the centrosome and in the cell periphery. In line with other kinesin-14 family members, KIFC3 may guide free microtubules to their destination at the bridge and/or may slide and crosslink central bridge microtubules in order to stage the cells for abscission.

KW - Abscission

KW - Cytokinesis

KW - KIFC3

KW - Kinesin-14

KW - Mitotic kinesin

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KIFC3 promotes mitotic progression and integrity of the central spindle in cytokinesis

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