Frontiers in Pharmacology (Apr 2018)

Development of Matrix Metalloproteinase-2 Inhibitors for Cardioprotection

  • Péter Bencsik,
  • Péter Bencsik,
  • Krisztina Kupai,
  • Anikó Görbe,
  • Anikó Görbe,
  • Éva Kenyeres,
  • Éva Kenyeres,
  • Zoltán V. Varga,
  • János Pálóczi,
  • Renáta Gáspár,
  • László Kovács,
  • Lutz Weber,
  • Ferenc Takács,
  • István Hajdú,
  • István Hajdú,
  • Gabriella Fabó,
  • Sándor Cseh,
  • László Barna,
  • László Barna,
  • Tamás Csont,
  • Csaba Csonka,
  • György Dormán,
  • Péter Ferdinandy,
  • Péter Ferdinandy

DOI
https://doi.org/10.3389/fphar.2018.00296
Journal volume & issue
Vol. 9

Abstract

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The objective of our present study is to develop novel inhibitors for MMP-2 for acute cardioprotection. In a series of pilot studies, novel substituted carboxylic acid derivatives were synthesized based on imidazole and thiazole scaffolds and then tested in a screeening cascade for MMP inhibition. We found that the MMP-inhibiting effects of imidazole and thiazole carboxylic acid-based compounds are superior in efficacy in comparison to the conventional hydroxamic acid derivatives of the same molecules. Based on these results, a 568-membered focused library of imidazole and thiazole compounds was generated in silico and then the library members were docked to the 3D model of MMP-2 followed by an in vitro medium throughput screening (MTS) based on a fluorescent assay employing MMP-2 catalytic domain. Altogether 45 compounds showed a docking score of >70, from which 30 compounds were successfully synthesized. Based on the MMP-2 inhibitory tests using gelatin zymography, 7 compounds were then selected and tested in neonatal rat cardiac myocytes subjected to simulated I/R injury. Six compounds showed significant cardio-cytoprotecion and the most effective compound (MMPI-1154) significantly decreased infarct size when applied at 1 μM in an ex vivo model for acute myocardial infarction. This is the first demonstration that imidazole and thiazole carboxylic acid-based compounds are more efficacious MMP-2 inhibitor than their hydroxamic acid derivatives. MMPI-1154 is a promising novel cardio-cytoprotective imidazole-carboxylic acid MMP-2 inhibitor lead candidate for the treatment of acute myocardial infarction.

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