Synthesis of novel quinine analogs and evaluation of their effects on Trypanosoma cruzi

Author:

Ceole Ligia F1,Gandhi Hirenkumar23,Villamizar Luz H4,Soares Maurilio J1,O'Sullivan Timothy P235

Affiliation:

1. Laboratory of Cell Biology, Carlos Chagas Institute/Fiocruz, 81350-010, Curitiba, PR, Brazil

2. School of Chemistry, University College Cork, Cork, T12 YN60, Ireland

3. Analytical & Biological Chemistry Research Facility, University College Cork, Cork, T12 YN60, Ireland

4. Laboratory of Molecular Biology of Trypanosomatids, Carlos Chagas Institute/Fiocruz, 81350-010, Curitiba, PR, Brazil

5. School of Pharmacy, University College Cork, Cork, T12 YN60, Ireland

Abstract

Aim: Chagas disease is a tropical disease caused by the hemoflagellate protozoan Trypanosoma cruzi. There is no vaccine for Chagas disease and available drugs (e.g., benznidazole) are effective only during the acute phase, displaying a variable curative activity in the established chronic form of the disease. New leads with high efficacy and better toxicity profiles are urgently required. Materials & methods: A library of novel quinine derivatives was synthesized using Heck chemistry and evaluated against the various developmental forms of T. cruzi. Results and Conclusion: Several novel quinine analogs with trypanocidal activity have been identified with the para-nitro-substituted derivative displaying a submicromolar IC50, which is 83-times lower than quinine and three-times lower than benznidazole. Transmission electron microscopy analysis demonstrated that these compounds induced a marked vacuolization of the kinetoplast of intracellular amastigotes and cell-derived trypomastigotes.

Publisher

Future Science Ltd

Subject

Drug Discovery,Pharmacology,Molecular Medicine

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