Molecules (Aug 2020)

Screening of Heteroaromatic Scaffolds against Cystathionine Beta-Synthase Enables Identification of Substituted Pyrazolo[3,4-c]Pyridines as Potent and Selective Orthosteric Inhibitors

  • Anna-Maria Fantel,
  • Vassilios Myrianthopoulos,
  • Anastasios Georgoulis,
  • Nikolaos Lougiakis,
  • Iliana Zantza,
  • George Lamprinidis,
  • Fiona Augsburger,
  • Panagiotis Marakos,
  • Constantinos E. Vorgias,
  • Csaba Szabo,
  • Nicole Pouli,
  • Andreas Papapetropoulos,
  • Emmanuel Mikros

DOI
https://doi.org/10.3390/molecules25163739
Journal volume & issue
Vol. 25, no. 16
p. 3739

Abstract

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Cystathionine β-synthase (CBS) is a key enzyme in the production of the signaling molecule hydrogen sulfide, deregulation of which is known to contribute to a range of serious pathological states. Involvement of hydrogen sulfide in pathways of paramount importance for cellular homeostasis renders CBS a promising drug target. An in-house focused library of heteroaromatic compounds was screened for CBS modulators by the methylene blue assay and a pyrazolopyridine derivative with a promising CBS inhibitory potential was discovered. The compound activity was readily comparable to the most potent CBS inhibitor currently known, aminoacetic acid, while a promising specificity over the related cystathionine γ-lyase was identified. To rule out any possibility that the inhibitor may bind the enzyme regulatory domain due to its high structural similarity with cofactor s-adenosylmethionine, differential scanning fluorimetry was employed. A sub-scaffold search guided follow-up screening of related compounds, providing preliminary structure-activity relationships with respect to requisites for efficient CBS inhibition by this group of heterocycles. Subsequently, a hypothesis regarding the exact binding mode of the inhibitor was devised on the basis of the available structure-activity relationships (SAR) and a deep neural networks analysis and further supported by induced-fit docking calculations.

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