The development of a structurally distinct series of BACE1 inhibitors via the (Z)-fluoro-olefin amide bioisosteric replacement

Michael J. Frohn,Longbin Liu,Aaron C. Siegmund,Wenyuan Qian,Albert Amegadzie,Ning Chen,Helming Tan,Dean Hickman,Stephen Wood,Paul H. Wen,Michael D. Bartberger,Douglas A. Whittington,Jennifer R. Allen,Matthew P. Bourbeau

The development of a structurally distinct series of BACE1 inhibitors via the (Z)-fluoro-olefin amide bioisosteric replacement

2020

Michael J. Frohn
Longbin Liu
Aaron C. Siegmund
Wenyuan Qian
Albert Amegadzie
Ning Chen
Helming Tan
Dean Hickman
Stephen Wood
Paul H. Wen
Michael D. Bartberger
Douglas A. Whittington
Jennifer R. Allen
Matthew P. Bourbeau

Abstract The (Z)-fluoro-olefin amide bioisosteric replacement is an effective tool for addressing various shortcomings of the parent amide. In an effort to fine tune ADME properties of BACE1 preclinical candidate AM-6494, a series of structurally distinct (Z)-fluoro-olefin containing analogs was developed that culminated in compound 15. Herein, we detail design considerations, synthetic challenges, structure activity relationship (SAR) studies, and in vivo properties of an advanced compound in this novel series of BACE1 inhibitors.

Keywords:

Structure–activity relationship
Amide
Organic chemistry
Combinatorial chemistry
Olefin fiber
ADME
Chemistry
Bioisostere

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