Cdk5 phosphorylation of its activators p35 and p39 determines subcellular location of the holokinase in a phosphorylation site-specific manner

Author:

Asada Akiko,Saito Taro,Hisanaga Shin-ichi

Abstract

Cdk5 is a member of the cyclin-dependent kinase (Cdk) family, which is activated by neuronal activator p35 or p39. Cdk5 regulates a variety of neuronal activities including neural migration, synaptic activity and neuronal death. p35 and p39 impart cytoplasmic membrane association of p35-Cdk5 and p39-Cdk5, respectively, through their myristoylation, but it is not clearly understood how the cellular localization is related to different functions. Here, we investigated the role of Cdk5 activity in the subcellular localization of p35-Cdk5 and p39-Cdk5. Cdk5 activity affected the localization of p35-Cdk5 and p39-Cdk5 via phosphorylation of p35 or p39. Using unphosphorylated or phosphomimetic mutants of p35 and p39, we found that phosphorylation at Ser8, common to p35 and p39, by Cdk5 regulated the cytoplasmic localization, perinuclear accumulation of unphosphorylated S8A mutants and whole cytoplasmic distribution of phosphomimetic S8E mutants. Cdk5 activity was necessary to retain Cdk5-activator complexes in the cytoplasm. Nevertheless, small but distinct amounts of p35 and p39 were detected in the nucleus. In particular, nuclear p35 and p39 were increased when the Cdk5 activity was inhibited. p39 had a propensity to accumulate in the nucleus more than p35, and phosphorylation at Thr84, specific to p39, regulated the potential nuclear localization activity of the Lys cluster in p39. These results suggest that the subcellular localization of the Cdk5-activator complexes is determined by its kinase activity, and also implicate a role for p39-Cdk5 in the nucleus.

Publisher

The Company of Biologists

Subject

Cell Biology

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