Molecules (Oct 2017)

Benzoic Acid Derivatives with Trypanocidal Activity: Enzymatic Analysis and Molecular Docking Studies toward Trans-Sialidase

  • Muhammad Kashif,
  • Antonio Moreno-Herrera,
  • Juan Carlos Villalobos-Rocha,
  • Benjamín Nogueda-Torres,
  • Jaime Pérez-Villanueva,
  • Karen Rodríguez-Villar,
  • José Lius Medina-Franco,
  • Peterson de Andrade,
  • Ivone Carvalho,
  • Gildardo Rivera

DOI
https://doi.org/10.3390/molecules22111863
Journal volume & issue
Vol. 22, no. 11
p. 1863

Abstract

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Chagas, or American trypanosomiasis, remains an important public health problem in developing countries. In the last decade, trans-sialidase has become a pharmacological target for new anti-Chagas drugs. In this work, the aims were to design and find a new series of benzoic acid derivatives as trans-sialidase (TS) inhibitors and anti-trypanosomal agents. Three compounds (14, 18, and 19) sharing a para-aminobenzoic acid moiety showed more potent trypanocidal activity than the commercially available drugs nifurtimox and benznidazole in both strains: the lysis concentration of 50% of the population (LC50) was <0.15 µM on the NINOA strain, and LC50 < 0.22 µM on the INC-5 strain. Additionally, compound 18 showed a moderate inhibition (47%) on the trans-sialidase enzyme and a binding model similar to DANA (pattern A).

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