Tyrosine hydroxylase expression and Cdk5 kinase activity in ataxic cerebellum

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Ataxia has been associated with abnormalities in neuronal differentiation and migration, which are regulated by Cyclin-dependent kinase 5 (Cdk5). The cerebellum of mice lacking Cdk5 or its activator, p35, resembles those of ataxic reeler and scrambler mice, suggesting that Cdk5 may contribute to ataxic pathology. As with other ataxic mice, the pogo/pogo mouse shows aberrant cerebellar tyrosine hydroxylase (TH) expression. Since Cdk5 phosphorylates and upregulates TH expression, we sought to analyze (i) Cdk5 activity in the pogo cerebellum, which exhibits abnormal TH expression, and (ii) TH expression in the cerebellum of p35-/- and p39-/- mice, which display reduced Cdk5 activity. Interestingly, we found that increased TH expression in the pogo cerebellum coincided with reduced Cdk5 activity. However, reduced Cdk5 activity in both p35-/- and p39-/- cerebellum did not correspond to defects in TH expression. Together, these suggest that abnormal TH expression in the cerebellum might be regulated by mechanisms other than Cdk5 activity.
Publisher
SPRINGER
Issue Date
2008-11
Language
English
Article Type
Article
Keywords

CYCLIN-DEPENDENT KINASE-5; PURKINJE-CELLS; MUTANT MOUSE; ABNORMAL EXPRESSION; MICE; GENE; POGO; NEURONS; IMMUNOREACTIVITY; PHOSPHORYLATION

Citation

MOLECULAR AND CELLULAR BIOCHEMISTRY, v.318, no.1-2, pp.7 - 12

ISSN
0300-8177
DOI
10.1007/s11010-008-9850-1
URI
http://hdl.handle.net/10203/87087
Appears in Collection
RIMS Journal Papers
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