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Synthesis and structure-activity relationship of potent, selective and orally active anthranilamide-based factor Xa inhibitors: application of weakly basic sulfoximine group as novel S4 binding element. | LitMetric

AI Article Synopsis

  • A new series of factor Xa inhibitors featuring a sulfoximine group as a unique binding component has been discovered within the anthranilamide chemotype.
  • Lead optimization of these compounds produced several highly effective anticoagulants in human plasma, with one standout compound, 18f, showing significant ex vivo prothrombin time prolongation in rats.
  • Comprehensive studies on compound 18f revealed a strong active metabolite, 18b, both of which exhibited remarkable effectiveness against arterial and venous thrombosis in rat models and selective action against similar serine proteases, leading to 18f being chosen for further research.

Article Abstract

A novel series of potent and efficacious factor Xa inhibitors which possesses sulfoximine moiety as novel S4 binding element in anthranilamide chemotype has been identified. Lead optimization at this novel P4 group led to many potent factor Xa inhibitors with excellent anticoagulant activity in human plasma. Selected compounds were dosed orally in rats and checked for their ex vivo prothrombin time prolonging activity, which resulted in identification of compound 5-chloro-N-(5-chloropyridin-2-yl)-2-(4-(N-(2-(diethylamino)acetyl)-S-methylsulfonimidoyl)benzamido)benzamide (18f). The detailed pharmacokinetic evaluation and subsequent metabolism study of 18f suggested the presence of an active metabolite. The compound 18f and its active metabolite 18b demonstrated excellent in vivo efficacy in both arterial and venous thrombosis model in rats and were found to be highly selective against related serine proteases. Based on this promising profile, compound 18f was selected for further evaluation.

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Source
http://dx.doi.org/10.1016/j.ejmech.2012.10.005DOI Listing

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