Science and Research

Drug repositioning as an effective therapy for protease-activated receptor 2 inhibition

Proteinase-activated receptor 2 (PAR-2) is a G protein-coupled receptor activated by both trypsin and a specific agonist peptide, SLIGKV-NH2. It has been linked to various pathologies, including pain and inflammation. Several peptide and peptidomimetic agonizts for PAR-2 have been developed exhibiting high potency and efficacy. However, the number of PAR-2 antagonists is smaller. We screened the Food and Drug Administration library of approved compounds to retrieve novel antagonists for repositioning in the PAR-2 structure. The most efficacious compound bicalutamide bound to the PAR-2 binding groove near the extracellular domain as observed in the in silico studies. Further, it showed reduced Ca(2+) release in trypsin activated cells in a dose-dependent manner. Hence, bicalutamide is a novel and potent PAR-2 antagonist which could be therapeutically useful in blocking multiple pathways diverging from PAR-2 signaling. Further, the novel scaffold of bicalutamide represents a new molecular structure for PAR-2 antagonism and can serve as a basis for further drug development.

  • Saqib, U.
  • Savai, R.
  • Liu, D.
  • Banerjee, S.
  • Baig, M. S.

Keywords

  • antagonist
  • drug repositioning
  • inflammation
  • proteinase-activated receptor 2
Publication details
DOI: 10.1002/jcb.27334
Journal: Journal of cellular biochemistry
Work Type: Original
Location: UGMLC
Disease Area: PALI
Partner / Member: MPI-BN
Access-Number: 30370939
See publication on PubMed

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