Synthesis of disubstituted amino acids and peptide inhibitors of amyloid beta aggregation

Identifier

etd-10302008-224954

Author

Gregory Todd McCandless, Louisiana State University and Agricultural and Mechanical CollegeFollow

Degree

Master of Science (MS)

Department

Chemistry

Document Type

Thesis

Abstract

The aggregation process of amyloid beta from monomeric peptide to oligomers and fibrils is believed to be connected with the neurological disorder Alzheimer’s disease. The focus of this research is the synthesis of alpha, alpha-disubstituted amino acids and peptide inhibitors of amyloid beta aggregation. The inhibitors are designed to interrupt (or alter) this process by binding to amyloid beta’s central hydrophobic core region (residues 17-20, Leucine-Valine- Phenylalanine-Phenylalanine). Target specificity is achieved via self recognition by basing the inhibitors on the sequence in this region. The inclusion of disubstituted amino acids in the sequence of the inhibitors will provide a blocking face (or side) to prevent further disease linked aggregation. This thesis describes the experimental investigations that were conducted to evaluate design elements that can be added to enhance inhibitor designs and methods for improving the synthesis of disubstituted amino acids.

Date

2008

Document Availability at the Time of Submission

Release the entire work immediately for access worldwide.

Recommended Citation

McCandless, Gregory Todd, "Synthesis of disubstituted amino acids and peptide inhibitors of amyloid beta aggregation" (2008). LSU Master's Theses. 643.
https://repository.lsu.edu/gradschool_theses/643

Committee Chair

Hammer, Robert P.

DOI

10.31390/gradschool_theses.643