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Cyclohexanehexol inhibitors of Abeta aggregation prevent and reverse Alzheimer phenotype in a mouse model
Authors:McLaurin JoAnne  Kierstead Meredith E  Brown Mary E  Hawkes Cheryl A  Lambermon Mark H L  Phinney Amie L  Darabie Audrey A  Cousins Julian E  French Janet E  Lan Melissa F  Chen Fusheng  Wong Sydney S N  Mount Howard T J  Fraser Paul E  Westaway David  St George-Hyslop Peter
Affiliation:Centre for Research in Neurodegenerative Diseases, 6 Queen's Park Crescent West, Toronto, Ontario M5S 3H2 Canada. j.mclaurin@utoronto.ca
Abstract:When given orally to a transgenic mouse model of Alzheimer disease, cyclohexanehexol stereoisomers inhibit aggregation of amyloid beta peptide (Abeta) into high-molecular-weight oligomers in the brain and ameliorate several Alzheimer disease-like phenotypes in these mice, including impaired cognition, altered synaptic physiology, cerebral Abeta pathology and accelerated mortality. These therapeutic effects, which occur regardless of whether the compounds are given before or well after the onset of the Alzheimer disease-like phenotype, support the idea that the accumulation of Abeta oligomers has a central role in the pathogenesis of Alzheimer disease.
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