Protein kinase C phosphorylates two of the four known syndecan cytoplasmic domains in vitro. Academic Article

abstract

• The transmembrane heparan sulfate proteoglycans of the syndecan family are implicated to participate in several cellular reactions which are dependent on protein kinase C. We have used an in vitro assay to assess whether any of the Peptides corresponding to the complete cytoplasmic domains of rat syndecans 1 through 4 were used as substrates for the enzyme. The syndecan-2 (fibroglycan) and syndecan-3 (N-syndecan) peptides were both found to be phosphorylated by protein kinase C with Kms of 15 +/- 3 microM and 85 +/- 25 microM, respectively, while the syndecan-1 and -4 peptides were not phosphorylated under the conditions used. The sites of in vitro phosphorylation for syndecans-2 and -3 were localized to ser-197 and ser-339, respectively. Thus, among 13 available sites (serines and threonines) in the four peptides, two were selectively modified by the enzyme. The specificity and the kinetics of the reactions indicate that the cytoplasmic domains of syndecan-2 and -3 are likely to be physiological substrates for protein kinase C.

authors

• Hook, Magnus

published proceedings

• Biochem Mol Biol Int

author list (cited authors)

• Prasthofer, T., Ek, B., Ekman, P., Owens, R., Hook, M., & Johansson, S.

citation count

• 20

complete list of authors

• Prasthofer, T||Ek, B||Ekman, P||Owens, R||Hook, M||Johansson, S

publication date

• July 1995

published in

• Biochem Mol Biol Int  Journal

keywords

• Amino Acid Sequence
• Animals
• Cytoplasm
• Kinetics
• Membrane Glycoproteins
• Molecular Sequence Data
• Peptide Fragments
• Phosphorylation
• Protein Kinase C
• Proteoglycans
• Rats
• Sequence Homology, Amino Acid
• Substrate Specificity
• Syndecan-1
• Syndecan-2
• Syndecan-3
• Syndecan-4
• Syndecans

PubMed Central ID

• 8528141

start page

• 793

end page

• 802

volume

• 36

issue

• 4