| Literature DB >> 15737955 |
Amy S Espeseth1, Min Xu, Qian Huang, Craig A Coburn, Kristen L G Jones, Marc Ferrer, Paul D Zuck, Berta Strulovici, Eric A Price, Guoxin Wu, Abigail L Wolfe, Janet E Lineberger, Mohinder Sardana, Katherine Tugusheva, Beth L Pietrak, Ming-Chih Crouthamel, Ming-Tain Lai, Elizabeth Chen Dodson, Renzo Bazzo, Xiao-Ping Shi, Adam J Simon, Yueming Li, Daria J Hazuda.
Abstract
Extracellular deposits of aggregated amyloid-beta (Abeta) peptides are a hallmark of Alzheimer disease; thus, inhibition of Abeta production and/or aggregation is an appealing strategy to thwart the onset and progression of this disease. The release of Abeta requires processing of the amyloid precursor protein (APP) by both beta- and gamma-secretase. Using an assay that incorporates full-length recombinant APP as a substrate for beta-secretase (BACE), we have identified a series of compounds that inhibit APP processing, but do not affect the cleavage of peptide substrates by BACE1. These molecules also inhibit the processing of APP and Abeta by BACE2 and selectively inhibit the production of Abeta(42) species by gamma-secretase in assays using CTF99. The compounds bind directly to APP, likely within the Abeta domain, and therefore, unlike previously described inhibitors of the secretase enzymes, their mechanism of action is mediated through APP. These studies demonstrate that APP binding agents can affect its processing through multiple pathways, providing proof of concept for novel strategies aimed at selectively modulating Abeta production.Entities:
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Year: 2005 PMID: 15737955 DOI: 10.1074/jbc.M414331200
Source DB: PubMed Journal: J Biol Chem ISSN: 0021-9258 Impact factor: 5.157