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Dynamin 2 Associates with Microtubules at Mitosis and Regulates Cell Cycle Progression
30
Citations
26
References
2010
Year
CytoskeletonCell CycleCellular PhysiologyDeletion MutantsCell RegulationEndocytic PathwayCell SignalingCell PhysiologyMolecular SignalingCell DivisionCell BiologyDynamin 2Membrane TrafficMicrotubule AssociationDevelopmental BiologySignal TransductionIntracellular TraffickingCellular BiochemistrySystems BiologyMedicineCell Development
Dynamin, a ~100 kDa large GTPase, is known as a key player for membrane traffic. Recent evidence shows that dynamin also regulates the dynamic instability of microtubules by a mechanism independent of membrane traffic. As microtubules are highly dynamic during mitosis, we investigated whether the regulation of microtubules by dynamin is essential for cell cycle progression. Dynamin 2 intensely localized at the mitotic spindle, and the localization depended on its proline-rich domain (PRD), which is required for microtubule association. The deletion of PRD resulted in the impairment of cytokinesis, whereby the mutant had less effect on endocytosis. Interestingly, dominant-negative dynamin (K44A), which blocks membrane traffic but has no effect on microtubules, also blocked cytokinesis. On the other hand, the deletion of the middle domain, which binds to γ-tubulin, impaired the entry into mitosis. As both deletion mutants had no significant effect on endocytosis, dynamin 2 may participate in cell cycle progression by regulating the microtubules. These data suggest that dynamin may play a key role for cell cycle progression by two distinct pathways, membrane traffic and cytoskeleton.
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