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PP6 regulation of Aurora A–TPX2 limits NDC80 phosphorylation and mitotic spindle size

Tomoaki Sobajima, Katarzyna M. Kowalczyk, Stefanos Skylakakis, Daniel Hayward, Luke J. Fulcher, Colette Neary, Caleb Batley, Samvid Kurlekar, Emile Roberts, Ulrike Grüneberg, Francis A. Barr

2023The Journal of Cell Biology20 citationsDOIOpen Access PDF

Abstract

Amplification of the mitotic kinase Aurora A or loss of its regulator protein phosphatase 6 (PP6) have emerged as drivers of genome instability. Cells lacking PPP6C, the catalytic subunit of PP6, have amplified Aurora A activity, and as we show here, enlarged mitotic spindles which fail to hold chromosomes tightly together in anaphase, causing defective nuclear structure. Using functional genomics to shed light on the processes underpinning these changes, we discover synthetic lethality between PPP6C and the kinetochore protein NDC80. We find that NDC80 is phosphorylated on multiple N-terminal sites during spindle formation by Aurora A-TPX2, exclusively at checkpoint-silenced, microtubule-attached kinetochores. NDC80 phosphorylation persists until spindle disassembly in telophase, is increased in PPP6C knockout cells, and is Aurora B-independent. An Aurora-phosphorylation-deficient NDC80-9A mutant reduces spindle size and suppresses defective nuclear structure in PPP6C knockout cells. In regulating NDC80 phosphorylation by Aurora A-TPX2, PP6 plays an important role in mitotic spindle formation and size control and thus the fidelity of cell division.

Topics & Concepts

KinetochoreAnaphaseSpindle checkpointCell biologyAurora B kinaseSpindle apparatusSpindle pole bodyMitosisBiologyMultipolar spindlesCell divisionCell cycleGeneticsCellChromosomeGeneMicrotubule and mitosis dynamicsPlant nutrient uptake and metabolismGenomics and Chromatin Dynamics
PP6 regulation of Aurora A–TPX2 limits NDC80 phosphorylation and mitotic spindle size | Litcius