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Article

Mediator Can Regulate Mitotic Entry and Direct Periodic Transcription in Fission Yeast

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Pages 4008-4018 | Received 18 Jun 2014, Accepted 18 Aug 2014, Published online: 20 Mar 2023
 

Abstract

Cdk8 is required for correct timing of mitotic progression in fission yeast. How the activity of Cdk8 is regulated is unclear, since the kinase is not activated by T-loop phosphorylation and its partner, CycC, does not oscillate. Cdk8 is, however, a component of the multiprotein Mediator complex, a conserved coregulator of eukaryotic transcription that is connected to a number of intracellular signaling pathways. We demonstrate here that other Mediator components regulate the activity of Cdk8 in vivo and thereby direct the timing of mitotic entry. Deletion of Mediator components Med12 and Med13 leads to higher cellular Cdk8 protein levels, premature phosphorylation of the Cdk8 target Fkh2, and earlier entry into mitosis. We also demonstrate that Mediator is recruited to clusters of mitotic genes in a periodic fashion and that the complex is required for the transcription of these genes. We suggest that Mediator functions as a hub for coordinated regulation of mitotic progression and cell cycle-dependent transcription. The many signaling pathways and activator proteins shown to function via Mediator may influence the timing of these cell cycle events.

SUPPLEMENTAL MATERIAL

Supplemental material for this article may be found at http://dx.doi.org/10.1128/MCB.00819-14.

ACKNOWLEDGMENTS

This work was supported by grants from the Swedish Research Council, the Swedish Cancer Society, the IngaBritt and Arne Lundberg Foundation, the Swedish Foundation for Strategic Research, and the Assar Gabrielsson Foundation.

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