Title of article
Conformational Restriction via Cyclization in β-Amyloid Peptide Aβ(1-28) Leads to an Inhibitor of Aβ(1-28) Amyloidogenesis and Cytotoxicity Original Research Article
Author/Authors
Aphrodite Kapurniotu، نويسنده , , Andreas Buck، نويسنده , , Marco Weber، نويسنده , , Anke Schmauder، نويسنده , , Thomas Hirsch، نويسنده , , Jürgen Bernhagen، نويسنده , , Marianna Tatarek-Nossol، نويسنده ,
Issue Information
ماهنامه با شماره پیاپی سال 2003
Pages
11
From page
149
To page
159
Abstract
The aggregation process of β-amyloid peptide Aβ into amyloid is strongly associated with the pathology of Alzheimerʹs disease (AD). Aggregation may involve a transition of an α helix in Aβ(1-28) into β sheets and interactions between residues 18–20 of the “Aβ amyloid core.” We applied an i, i+4 cyclic conformational constraint to the Aβ amyloid core and devised side chain-to-side chain lactam-bridged cyclo17, 21-[Lys17, Asp21]Aβ(1-28). In contrast to Aβ(1-28) and [Lys17, Asp21]Aβ(1-28), cyclo17, 21-[Lys17, Asp21]Aβ(1-28) was not able to form β sheets and cytotoxic amyloid aggregates. Cyclo17, 21-[Lys17, Asp21]Aβ(1-28) was able to interact with Aβ(1-28) and to inhibit amyloid formation and cytotoxicity. Cyclo17, 21-[Lys17, Asp21]Aβ(1-28) also interacted with Aβ(1-40) and interfered with its amyloidogenesis. Cyclo17, 21-[Lys17, Asp21]Aβ(1-28) or similarly constrained Aβ sequences may find therapeutic and diagnostic applications in AD.
Journal title
Chemistry and Biology
Serial Year
2003
Journal title
Chemistry and Biology
Record number
1158611
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