Design of potent inhibitors of human beta-secretase. Part 2.

John N. Freskos,Yvette M. Fobian,Timothy E. Benson,Joseph B. Moon,Michael J. Bienkowski,David L. Brown,Thomas L. Emmons,Robert M. Heintz,Alice L. Laborde,Joseph J. McDonald,Brent V. Mischke,John M. Molyneaux,Patrick B. Mullins,D. Bryan Prince,Donna J. Paddock,Alfredo G. Tomasselli,Greg Winterrowd

Design of potent inhibitors of human beta-secretase. Part 2.

2007

John N. Freskos
Yvette M. Fobian
Timothy E. Benson
Joseph B. Moon
Michael J. Bienkowski
David L. Brown
Thomas L. Emmons
Robert M. Heintz
Alice L. Laborde
Joseph J. McDonald
Brent V. Mischke
John M. Molyneaux
Patrick B. Mullins
D. Bryan Prince
Donna J. Paddock
Alfredo G. Tomasselli
Greg Winterrowd

Abstract We describe an optimized series of acyclic hydroxyethylamine transition state isosteres of β-secretase that incorporates a variety of P 2 side chains that yield potent inhibitors with excellent cellular activity. A 2.2 A crystal structure of compound 13 is shown.

Keywords:

Side chain
Amyloid precursor protein secretase
Stereochemistry
Hydrolase
Chemistry
Biochemistry
Structure–activity relationship
β secretase
Beta (finance)
cellular activity
Combinatorial chemistry
Protein structure

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