Characterization of PDZ-binding kinase, a mitotic kinase.

Proc Natl Acad Sci U S A

Department of Molecular and Cellular Biology, Harvard University, 16 Divinity Avenue, Cambridge, MA 02138, USA.

Published: May 2000

AI Article Synopsis

  • hDlg, a human version of the Drosophila Discs-large tumor suppressor, interacts with the APC tumor suppressor and HPV E6 protein, indicating its role in cancer biology.
  • A new serine/threonine kinase called PBK was identified that binds to hDlg's PDZ2 domain; its mRNA is mainly found in the placenta rather than in the adult brain.
  • PBK and hDlg are phosphorylated during mitosis in HeLa cells, with PBK's phosphorylation being essential for its kinase activity, suggesting PBK may connect hDlg to cell cycle regulation and signaling pathways.

Article Abstract

hDlg, the human homologue of the Drosophila Discs-large (Dlg) tumor suppressor protein, is known to interact with the tumor suppressor protein APC and the human papillomavirus E6 transforming protein. In a two-hybrid screen, we identified a 322-aa serine/threonine kinase that binds to the PDZ2 domain of hDlg. The mRNA for this PDZ-binding kinase, or PBK, is most abundant in placenta and absent from adult brain tissue. The protein sequence of PBK has all the characteristic protein kinase subdomains and a C-terminal PDZ-binding T/SXV motif. In vitro, PBK binds specifically to PDZ2 of hDlg through its C-terminal T/SXV motif. PBK and hDlg are phosphorylated at mitosis in HeLa cells, and the mitotic phosphorylation of PBK is required for its kinase activity. In vitro, cdc2/cyclin B phosphorylates PBK. This evidence shows how PBK could link hDlg or other PDZ-containing proteins to signal transduction pathways regulating the cell cycle or cellular proliferation.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC25800PMC
http://dx.doi.org/10.1073/pnas.090102397DOI Listing

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