Microorganisms (Feb 2021)

Identification of <i>Trypanosoma cruzi</i> Growth Inhibitors with Activity In Vivo within a Collection of Licensed Drugs

  • Nieves Martinez-Peinado,
  • Nuria Cortes-Serra,
  • Julian Sherman,
  • Ana Rodriguez,
  • Juan M. Bustamante,
  • Joaquim Gascon,
  • Maria-Jesus Pinazo,
  • Julio Alonso-Padilla

DOI
https://doi.org/10.3390/microorganisms9020406
Journal volume & issue
Vol. 9, no. 2
p. 406

Abstract

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Chagas disease, caused by the parasite Trypanosoma cruzi (T. cruzi), affects more than six million people worldwide, with its greatest burden in Latin America. Available treatments present frequent toxicity and variable efficacy at the chronic phase of the infection, when the disease is usually diagnosed. Hence, development of new therapeutic strategies is urgent. Repositioning of licensed drugs stands as an attractive fast-track low-cost approach for the identification of safer and more effective chemotherapies. With this purpose we screened 32 licensed drugs for different indications against T. cruzi. We used a primary in vitro assay of Vero cells infection by T. cruzi. Five drugs showed potent activity rates against it (IC50 −1), which were also specific (selectivity index >15) with respect to host cells. T. cruzi inhibitory activity of four of them was confirmed by a secondary anti-parasitic assay based on NIH-3T3 cells. Then, we assessed toxicity to human HepG2 cells and anti-amastigote specific activity of those drugs progressed. Ultimately, atovaquone-proguanil, miltefosine, and verapamil were tested in a mouse model of acute T. cruzi infection. Miltefosine performance in vitro and in vivo encourages further investigating its use against T. cruzi.

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