Discovery and gram-scale synthesis of BMS-593214, a potent, selective FVIIa inhibitor

E. Scott Priestley,Indawati De Lucca,Jinglan Zhou,Jiacheng Zhou,Eddine Saiah,Robert V. Stanton,Leslie Robinson,Joseph M. Luettgen,Anzhi Wei,Xiao Wen,Robert M. Knabb,Pancras C. Wong,Ruth R. Wexler

Discovery and gram-scale synthesis of BMS-593214, a potent, selective FVIIa inhibitor

2013

E. Scott Priestley
Indawati De Lucca
Jinglan Zhou
Jiacheng Zhou
Eddine Saiah
Robert V. Stanton
Leslie Robinson
Joseph M. Luettgen
Anzhi Wei
Xiao Wen
Robert M. Knabb
Pancras C. Wong
Ruth R. Wexler

Abstract A 6-amidinotetrahydroquinoline screening hit was driven to a structurally novel, potent, and selective FVIIa inhibitor through a combination of library synthesis and rational design. An efficient gram-scale synthesis of the active enantiomer BMS-593214 was developed, which required significant optimization of the key Povarov annulation. Importantly, BMS-593214 showed antithrombotic efficacy in a rabbit arterial thrombosis model. A crystal structure of BMS-593214 bound to FVIIa highlights key contacts with Asp 189, Lys 192, and the S2 pocket.

Keywords:

Antithrombotic
Rational design
Benzamidine
Stereochemistry
Organic chemistry
Enantiomer
Chemistry
Annulation
Biochemistry
Coagulation factor VIIa

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