Design and synthesis of cell potent BACE-1 inhibitors: Structure–activity relationship of P1′ substituents

Article ID	Journal	Published Year	Pages	File Type
1372726	Bioorganic & Medicinal Chemistry Letters	2009	6 Pages	PDF

Abstract

Using structure-guided design, hydroxyethylamine BACE-1 inhibitors were optimized to nanomolar Aβ cellular inhibition with selectivity against cathepsin-D. X-ray crystallography illuminated the S1′ residues critical to this effort, which culminated in compounds 56 and 57 that exhibited potency and selectivity but poor permeability and high P-gp efflux.

Graphical abstractUsing structure-guided design, hydroxyethylamine BACE-1 inhibitors were optimized to nanomolar Aβ cellular inhibition with selectivity against cathepsin-D. X-ray crystallography illuminated the S1′ residues critical to this effort, which culminated in compounds 56 and 57 that exhibited potency and selectivity but poor permeability and high P-gp efflux.Figure optionsDownload full-size imageDownload as PowerPoint slide

Keywords

Alzheimer?s disease

Related Topics

Physical Sciences and Engineering Chemistry Organic Chemistry

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Design and synthesis of cell potent BACE-1 inhibitors: Structure–activity relationship of P1′ substituents

Authors

Jennifer M. Sealy, Anh P. Truong, Luke Tso, Gary D. Probst, Jose Aquino, Roy K. Hom, Barbara M. Jagodzinska, Darren Dressen, David W.G. Wone, Louis Brogley, Varghese John, Jay S. Tung, Michael A. Pleiss, John A. Tucker, Andrei W. Konradi,