Sb. Vyas et Lk. Duffy, STABILIZATION OF SECONDARY STRUCTURE OF ALZHEIMER P-PROTEIN BY ALUMINUM(III) IONS AND D-ASP SUBSTITUTIONS, Biochemical and biophysical research communications, 206(2), 1995, pp. 718-723
The CD spectra of the D-Asp substituted analogs of amyloid peptides, b
eta 6-25 and beta 1-40, showed a distinct blue-shift on A1(3+) complex
ation. The influence of Al3+ coordination was most significant on the
triply substituted beta 1-40 (D-Asp (1,7,23)). This analog showed a re
duction of the minima near 210nm and a simultaneous increase in the ma
xima near 200nm as compared to the native L-Asp beta 1-40. These obser
vations suggest that Al3+ interaction with D-Asp induces the peptide b
ackbone to increase its antiparallel beta-sheet character. D-Asp subst
itution and chelation by A(l3+) lead to increased stability of higher
molecular weight species of beta 1-40, and thereby could increase the
toxicity of the Alzheimer amyloid protein. (C) 1995 Academic Press, In
c.