Discovery of a Potent Parenterally Administered Factor XIa Inhibitor with Hydroxyquinolin-2(1H)-one as the P2′ Moiety

Zilun Hu,Pancras C. Wong,Paul J. Gilligan,Wei Han,Kumar Balashanmuga Pabbisetty,Jeffrey M. Bozarth,Earl J. Crain,Timothy W. Harper,Joseph M. Luettgen,Joseph E. Myers,Vidhyashankar Ramamurthy,Karen A. Rossi,Steven Sheriff,Carol A. Watson,Anzi Wei,Joanna J. Zheng,Dietmar A. Seiffert,Ruth R. Wexler,Mimi L. Quan

Discovery of a Potent Parenterally Administered Factor XIa Inhibitor with Hydroxyquinolin-2(1H)-one as the P2′ Moiety

2015

Zilun Hu
Pancras C. Wong
Paul J. Gilligan
Wei Han
Kumar Balashanmuga Pabbisetty
Jeffrey M. Bozarth
Earl J. Crain
Timothy W. Harper
Joseph M. Luettgen
Joseph E. Myers
Vidhyashankar Ramamurthy
Karen A. Rossi
Steven Sheriff
Carol A. Watson
Anzi Wei
Joanna J. Zheng
Dietmar A. Seiffert
Ruth R. Wexler
Mimi L. Quan

Structure–activity relationship optimization of phenylalanine P1′ and P2′ regions with a phenylimidazole core resulted in a series of potent FXIa inhibitors. Introducing 4-hydroxyquinolin-2-one as the P2′ group enhanced FXIa affinity and metabolic stability. Incorporation of an N-methyl piperazine amide group to replace the phenylalanine improved both FXIa potency and aqueous solubility. Combination of the optimization led to the discovery of FXIa inhibitor 13 with a FXIa Ki of 0.04 nM and an aPTT EC2x of 1.0 μM. Dose-dependent efficacy (EC50 of 0.53 μM) was achieved in the rabbit ECAT model with minimal bleeding time prolongation.

Keywords:

Solubility
Pharmacology
Biology
Potency
Amide
Phenylalanine
Moiety
Bleeding time
EC50
Piperazine
Factor XIa

Correction
Source
Cite
Save
Machine Reading By IdeaReader

References

Citations