Macrocyclic Inhibitors of β-Secretase: Functional Activity in an Animal Model

Shawn J. Stachel,Craig A. Coburn,Sethu Sankaranarayanan,Eric A. Price,Beth Pietrak,Qian Huang,Janet Lineberger,Amy S. Espeseth,Lixia Jin,Joan D. Ellis,M. Katharine Holloway,Sanjeev Munshi,Timothy J. Allison,Daria J. Hazuda,Adam J. Simon,Samuel L. Graham,Joseph P. Vacca

Macrocyclic Inhibitors of β-Secretase: Functional Activity in an Animal Model

2006

Shawn J. Stachel
Craig A. Coburn
Sethu Sankaranarayanan
Eric A. Price
Beth Pietrak
Qian Huang
Janet Lineberger
Amy S. Espeseth
Lixia Jin
Joan D. Ellis
M. Katharine Holloway
Sanjeev Munshi
Timothy J. Allison
Daria J. Hazuda
Adam J. Simon
Samuel L. Graham
Joseph P. Vacca

A macrocyclic inhibitor of β-secretase was designed by covalently cross-linking the P1 and P3 side chains of an isophthalamide-based inhibitor. Macrocyclization resulted in significantly improved potency and physical properties when compared to the initial lead structures. More importantly, these macrocyclic inhibitors also displayed in vivo amyloid lowering when dosed in a murine model.

Keywords:

Amyloid precursor protein secretase
Enzyme
Chemical synthesis
In vivo
Amyloid precursor protein
Organic chemistry
Amyloid
Biological activity
Stereochemistry
Biochemistry
Chemistry
Enzyme inhibitor
Lactam

Correction
Source
Cite
Save
Machine Reading By IdeaReader

References

Citations