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Plk1 regulates spindle orientation by phosphorylating NuMA in human cells.

Life science alliance (2018-11-21)
Shrividya Sana, Riya Keshri, Ashwathi Rajeevan, Sukriti Kapoor, Sachin Kotak
ANOTACE

Proper orientation of the mitotic spindle defines the correct division plane and is essential for accurate cell division and development. In metazoans, an evolutionarily conserved complex comprising of NuMA/LGN/Gαi regulates proper orientation of the mitotic spindle by orchestrating cortical dynein levels during metaphase. However, the molecular mechanisms that modulate the spatiotemporal dynamics of this complex during mitosis remain elusive. Here, we report that acute inactivation of Polo-like kinase 1 (Plk1) during metaphase enriches cortical levels of dynein/NuMA/LGN and thus influences spindle orientation. We establish that this impact of Plk1 on cortical levels of dynein/NuMA/LGN is through NuMA, but not via dynein/LGN. Moreover, we reveal that Plk1 inhibition alters the dynamic behavior of NuMA at the cell cortex. We further show that Plk1 directly interacts and phosphorylates NuMA. Notably, NuMA-phosphorylation by Plk1 impacts its cortical localization, and this is needed for precise spindle orientation during metaphase. Overall, our finding connects spindle-pole pool of Plk1 with cortical NuMA and answers a long-standing puzzle about how spindle-pole Plk1 gradient dictates proper spindle orientation for error-free mitosis.

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Sigma-Aldrich
Plk1 Protein, active, 10 µg, Active, N-terminal 6His tagged, recombinant, human Plk1. For use in Kinase Assays.
Sigma-Aldrich
Anti-GPSM2 antibody produced in rabbit, affinity isolated antibody, buffered aqueous glycerol solution