Determinants for Activation of the Atypical AGC Kinase Greatwall during M Phase Entry

Author:

Blake-Hodek Kristina A.1,Williams Byron C.1,Zhao Yong1,Castilho Priscila V.1,Chen Wei1,Mao Yuxin1,Yamamoto Tomomi M.2,Goldberg Michael L.1

Affiliation:

1. Department of Molecular Biology and Genetics, Cornell University, Ithaca, New York, USA

2. Department of Pharmacology, University of Colorado School of Medicine, Aurora, Colorado, USA

Abstract

ABSTRACT The atypical AGC kinase Greatwall (Gwl) mediates a pathway that prevents the precocious removal of phosphorylations added to target proteins by M phase-promoting factor (MPF); Gwl is thus essential for M phase entry and maintenance. Gwl itself is activated by M phase-specific phosphorylations that are investigated here. Many phosphorylations are nonessential, being located within a long nonconserved region, any part of which can be deleted without effect. Using mass spectrometry and mutagenesis, we have identified 3 phosphorylation sites (phosphosites) critical to Gwl activation (pT193, pT206, and pS883 in Xenopus laevis ) located in evolutionarily conserved domains that differentiate Gwl from related kinases. We propose a model in which the initiating event for Gwl activation is phosphorylation by MPF of the proline-directed sites T193 and T206 in the presumptive activation loop. After this priming step, Gwl can intramolecularly phosphorylate its C-terminal tail at pS883; this site probably plays a role similar to that of the tail/Z motif of other AGC kinases. These events largely (but not completely) explain the full activation of Gwl at M phase.

Publisher

American Society for Microbiology

Subject

Cell Biology,Molecular Biology

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