Regarding deposition of amyloid β-protein (Aβ) in brains with Alzheimer’s disease
(AD), we previously identified a novel Aβ species that strongly binds to GM1 ganglioside
(GM1) in human brains that exhibit early pathological changes of AD. We hypothesized
that Aβ undergoes conformational alteration through its binding to GM1 and acts as
a seed. We recently found that an increase in the cholesterol concentration in host
membranes markedly accelerates Aβ binding to GM1. We then investigated whether the
cholesterol concentration in neuronal membranes could be altered under biological
conditions that are associated with risk factors for AD development. We attempted
to determine the distribution of cholesterol in the synaptic plasma membranes (SPMs)
of human apolipoprotein E (apoE)-knock-in mice and found that the cholesterol concentration
in the exofacial leaflet of SPMs of the human apoE4-knock-in mice was approximately
twice that of human apoE3-knock-in mice. The results of our studies suggest that an
increase in the cholesterol concentration in the neuronal membranes accelerates Aβ
aggregation through the formation of an endogenous seed.
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Katsuhiko Yanagisawa, M.D.
Department of Dementia Research
National Institute for Longevity Sciences
36-3 Gengo
Morioka
Obu
Japan
474-8522
Phone: 81-562-44-5651 (ext. 834)
Fax: 81-562-44-6594
Email: katuhiko@nils.go.jp