Journal
ELECTROPHORESIS
Volume 25, Issue 20, Pages 3336-3343Publisher
WILEY
DOI: 10.1002/elps.200406068
Keywords
Alzheimer's disease; amyloid beta; neurodegeneration; plasma
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In this prospective study, for the first time we have separated and quantified amyloid P (AD) peptides in the plasma of patients with Alzheimer's disease (AD, n = 8) and ageand environment-matched healthy controls (n = 9) with urea-based Abeta-sodium dodecyl sulfate-polyacrylamicle gel electrophoresis (SDS-PAGE)/immunoblot. In addition to the AD peptides 1-37/38/39/40/42, which we recently identified as regular constituents of human cerebrospinal fluid (CSF), we have observed a novel electrophoretic band migrating slightly cathodically to Abeta1 -42. Since a standard peptide with the amino acid sequence Abeta2-40 migrates in the same position, we hypothesize that this plasma-specific band may correspond to Abeta2-40. The concentration of Abeta peptides in the plasma has been approximately 100-fold lower compared to the CSF. Interestingly, the concentration of the two shortest peptides and the longest one of these considered here (i.e., Abeta1-37/38/42) have increased significantly when the samples have been frozen at -80degreesC before immunoprecipitation, while the 'middle-length' peptides (i.e., Abeta1-39/40) have not been affected by this procedure. We have not observed significant differences of the Abeta peptides concentrations between AD and control subjects. Our method can be used to investigate the significance of plasma Abeta pepticles in neurodegenerative disorders, and to monitor the efficiency of drugs with beta/-Y-secretase inhibitory potency.
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