Proline-directed phosphorylation of human Tau protein

Richard Vulliet; S Mitchell Halloran; Ruedi K Braun; Alan J Smith; Gloria Lee

doi:10.1016/S0021-9258(18)41710-3

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Proline-directed phosphorylation of human Tau protein

Journal article

Open access

Peer reviewed

Proline-directed phosphorylation of human Tau protein

Richard Vulliet, S Mitchell Halloran, Ruedi K Braun, Alan J Smith and Gloria Lee

The Journal of biological chemistry, Vol.267(31), pp.22570-22574

1992

DOI: 10.1016/S0021-9258(18)41710-3

PMID: 1429606

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Abstract

The primary sequence of the microtubule-associated protein tau contains multiple repeats of the sequence -X-Ser/Thr-Pro-X-, the consensus sequence for the proline-directed protein kinase (p34cdc2/p58cyclin A). When phosphorylated by proline-directed protein kinase in vitro, tau was found to incorporate up to 4.4 mol of phosphate/mol of protein. Isoelectric focusing of the tryptic phosphopeptides demonstrated the presence of five distinct peptides with pI values of approximately 6.9, 6.5, 5.6-5.9, 4.7, and 3.6. Mapping of the tryptic phosphopeptides by high performance liquid chromatography techniques demonstrated three distinct peaks. Data from gas phase sequencing, amino acid analysis, and phosphoamino acid analysis suggest that proline-directed protein kinase phosphorylates tau at four sites. Each site demonstrates the presence of a proline residue on the carboxyl-terminal side of the phosphorylated residue. Two phosphorylation sites are located adjacent to the three-repeat microtubule-binding domain that has been found to be required for the in vivo co-localization of tau protein to microtubules. Two other putative phosphorylation sites are located within the identified epitope of the monoclonal antibody Tau-1. Phosphorylation of these sites altered the immunoreactivity of tau to Tau-1 antibody. Since the neuronal microtubule-associated protein tau is multiply phosphorylated in Alzheimer's disease, and Tau-1 immunoreactivity is similarly reduced in neurofibrillary tangles and enhanced after dephosphorylation, phosphorylation at one or more of these sites may correlate with abnormally phosphorylated sites in tau protein in Alzheimer's disease.

Fundamental and applied biological sciences. Psychology

Biological and medical sciences

Cytoskeleton, cytoplasm. Intracellular movements

Molecular and cellular biology

Cell structures and functions

Details

Title: Subtitle: Proline-directed phosphorylation of human Tau protein
Creators: Richard Vulliet - Univ. California, school veterinary medicine, dep. veterinary pharmacology toxicology, Davis CA 95616, United States
S Mitchell Halloran - Univ. California, school veterinary medicine, dep. veterinary pharmacology toxicology, Davis CA 95616, United States
Ruedi K Braun - Univ. California, school veterinary medicine, dep. veterinary pharmacology toxicology, Davis CA 95616, United States
Alan J Smith - Univ. California, school veterinary medicine, dep. veterinary pharmacology toxicology, Davis CA 95616, United States
Gloria Lee - Univ. California, school veterinary medicine, dep. veterinary pharmacology toxicology, Davis CA 95616, United States
Resource Type: Journal article
Publication Details: The Journal of biological chemistry, Vol.267(31), pp.22570-22574
DOI: 10.1016/S0021-9258(18)41710-3
PMID: 1429606
NLM abbreviation: J Biol Chem
ISSN: 0021-9258
eISSN: 1083-351X
Publisher: American Society for Biochemistry and Molecular Biology; Bethesda, MD
Language: English
Date published: 1992
Academic Unit: Iowa Neuroscience Institute; Immunology; Internal Medicine
Record Identifier: 9984065493702771

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