| Literature DB >> 27807285 |
Matthew E Kennedy1, Andrew W Stamford2, Xia Chen3, Kathleen Cox4, Jared N Cumming5, Marissa F Dockendorf4, Michael Egan6, Larry Ereshefsky7, Robert A Hodgson3, Lynn A Hyde3, Stanford Jhee7, Huub J Kleijn4, Reshma Kuvelkar3, Wei Li5, Britta A Mattson8, Hong Mei4, John Palcza9, Jack D Scott5, Michael Tanen10, Matthew D Troyer11, Jack L Tseng11, Julie A Stone4, Eric M Parker1, Mark S Forman12.
Abstract
β-Amyloid (Aβ) peptides are thought to be critically involved in the etiology of Alzheimer's disease (AD). The aspartyl protease β-site amyloid precursor protein cleaving enzyme 1 (BACE1) is required for the production of Aβ, and BACE1 inhibition is thus an attractive target for the treatment of AD. We show that verubecestat (MK-8931) is a potent, selective, structurally unique BACE1 inhibitor that reduced plasma, cerebrospinal fluid (CSF), and brain concentrations of Aβ40, Aβ42, and sAPPβ (a direct product of BACE1 enzymatic activity) after acute and chronic administration to rats and monkeys. Chronic treatment of rats and monkeys with verubecestat achieved exposures >40-fold higher than those being tested in clinical trials in AD patients yet did not elicit many of the adverse effects previously attributed to BACE inhibition, such as reduced nerve myelination, neurodegeneration, altered glucose homeostasis, or hepatotoxicity. Fur hypopigmentation was observed in rabbits and mice but not in monkeys. Single and multiple doses were generally well tolerated and produced reductions in Aβ40, Aβ42, and sAPPβ in the CSF of both healthy human subjects and AD patients. The human data were fit to an amyloid pathway model that provided insight into the Aβ pools affected by BACE1 inhibition and guided the choice of doses for subsequent clinical trials.Entities:
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Year: 2016 PMID: 27807285 DOI: 10.1126/scitranslmed.aad9704
Source DB: PubMed Journal: Sci Transl Med ISSN: 1946-6234 Impact factor: 17.956