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Discovery of Potent and Selective Quinoxaline-Based Protease-Activated Receptor 4 (PAR4) Antagonists for the Prevention of Arterial Thrombosis.

Xiaojun ZhangWen JiangJeremy M RichterJ Alex BatesSamuel K ReznikSylwia StachuraRichard RampullaDyamanna DoddalingappaSankar UlaganathanJi HuaJeffrey S BostwickChi SumShana PosySarah MalmstromJoyce DickeyDavid HardenR Michael LawrenceVictor R GuarinoWilliam A SchumacherPancras WongJing YangDavid A GordonRuth R WexlerE Scott Priestley
Published in: Journal of medicinal chemistry (2024)
PAR4 is a promising antithrombotic target with potential for separation of efficacy from bleeding risk relative to current antiplatelet therapies. In an effort to discover a novel PAR4 antagonist chemotype, a quinoxaline-based HTS hit 3 with low μM potency was identified. Optimization of the HTS hit through the use of positional SAR scanning and the design of conformationally constrained cores led to the discovery of a quinoxaline-benzothiazole series as potent and selective PAR4 antagonists. The lead compound 48 , possessing a 2 nM IC 50 against PAR4 activation by γ-thrombin in platelet-rich plasma (PRP) and greater than 2500-fold selectivity versus PAR1, demonstrated robust antithrombotic efficacy and minimal bleeding in the cynomolgus monkey models.
Keyphrases
  • platelet rich plasma
  • atrial fibrillation
  • small molecule
  • high throughput
  • pulmonary embolism
  • mass spectrometry
  • structural basis