| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 2040525 | Cell Reports | 2016 | 14 Pages |
•Unperturbed mitosis is relatively normal in p31comet- and TRIP13-deficient human cells•MAD2 inactivation and mitotic exit are partially impaired without p31comet•TRIP13-deficient cells contain only C-MAD2•TRIP13-deficient cells are unable to activate the spindle-assembly checkpoint
SummaryBiochemical studies have indicated that p31comet and TRIP13 are critical for inactivating MAD2. To address unequivocally whether p31comet and TRIP13 are required for mitotic exit at the cellular level, their genes were ablated either individually or together in human cells. Neither p31comet nor TRIP13 were absolutely required for unperturbed mitosis. MAD2 inactivation was only partially impaired in p31comet-deficient cells. In contrast, TRIP13-deficient cells contained MAD2 exclusively in the C-MAD2 conformation. Our results indicate that although p31comet enhanced TRIP13-mediated MAD2 conversion, it was not absolutely necessary for the process. Paradoxically, TRIP13-deficient cells were unable to activate the spindle-assembly checkpoint, revealing that cells lacking the ability to inactivate MAD2 were incapable in mounting a checkpoint response. These results establish a paradigm of the roles of p31comet and TRIP13 in both checkpoint activation and inactivation.
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