Tyrosine Phosphorylation of the p21 Cyclin-dependent Kinase Inhibitor Facilitates the Development of Proneural Glioma |
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| Authors: | Ellen Hukkelhoven Yuhui Liu Nancy Yeh Daniel Ciznadija Stacy W Blain Andrew Koff |
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| Institution: | From the ‡Gerstner School of Biomedical Sciences and ;§Sloan-Kettering Institute, Memorial Sloan-Kettering Cancer Center, New York, New York 10021 and ;the ¶Departments of Pediatrics and Anatomy and Cell Biology, SUNY Downstate Medical Center, Brooklyn, New York 11203 |
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| Abstract: | Phosphorylation of Tyr-88/Tyr-89 in the 310 helix of p27 reduces its cyclin-dependent kinase (CDK) inhibitory activity. This modification does not affect the interaction of p27 with cyclin-CDK complexes but does interfere with van der Waals and hydrogen bond contacts between p27 and amino acids in the catalytic cleft of the CDK. Thus, it had been suggested that phosphorylation of this site could switch the tumor-suppressive CDK inhibitory activity to an oncogenic activity. Here, we examined this hypothesis in the RCAS-PDGF-HA/nestin-TvA proneural glioma mouse model, in which p21 facilitates accumulation of nuclear cyclin D1-CDK4 and promotes tumor development. In these tumor cells, approximately one-third of the p21 is phosphorylated at Tyr-76 in the 310 helix. Mutation of this residue to glutamate reduced inhibitory activity in vitro. Mutation of this residue to phenylalanine reduced the tumor-promoting activity of p21 in the animal model, whereas glutamate or alanine substitution allowed tumor formation. Consequently, we conclude that tyrosine phosphorylation contributes to the conversion of CDK inhibitors from tumor-suppressive roles to oncogenic roles. |
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| Keywords: | Animal Models Cancer Biology CDK (Cyclin-dependent Kinase) Cell Proliferation Glioblastoma RCAS-PDGF-HA/nestin-TvA Mouse Model CDK Inhibitors p21Waf1/Cip1 Proneural Glioma Tyrosine Phosphorylation |
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