Formation of a membrane-active form of amyloid β-protein in raft-like model membranes

The conversion of soluble, nontoxic amyloid beta-protein (Abeta) to aggregated, toxic Abeta rich in beta-sheet structures is considered to be the key step in the development of Alzheimer's disease. We have proposed that the aggregation proceeds in the lipid raft containing a ganglioside cluster, the formation of which is facilitated by cholesterol and for which Abeta shows a specific affinity. In this study, using fluorescence resonance energy transfer, we found that after Abeta binds to raft-like membranes composed of monosialoganglioside GM1/cholesterol/sphingomyelin (1/1/1), the protein can translocate to the phosphatidylcholine membranes to which soluble Abeta does not bind. Furthermore, self-quenching experiments using fluorescein-labeled Abeta revealed that the translocation process competes with the oligomerization of the protein in the raft-like membranes. These results suggest that the lipid raft containing a ganglioside cluster serves as a conformational catalyst or a chaperon generating a membrane-active form of Abeta with seeding ability. (C) 2003 Elsevier Science (USA). All rights reserved.