In vitro and in vivo antileishmanial activity of thioridazine

Author:

Rodríguez Sergio Sifontes1ORCID,Mollineda-Diogo Niurka2,Monzote-Fidalgo Lianet3,Escalona-Montaño Alma Reyna1,García-Trevijano José Antonio Escario4,Aguirre-García María Magdalena1,Meneses-Marcel Alfredo Irenaldo2

Affiliation:

1. UNAM Facultad de Medicina: Universidad Nacional Autonoma de Mexico Facultad de Medicina

2. Center of Bioactive Chemicals

3. IPK: Instituto de Medicina Tropical Pedro Kouri

4. Universidad Complutense de Madrid Facultad de Farmacia

Abstract

Abstract Leishmaniasis is a neglected disease with high prevalence and incidence in tropical and subtropical areas. Existing drugs are limited due to cost, toxicity, declining efficacy and unavailability in endemic places. Drug repurposing has established as an efficient way for the discovery of drugs for a variety of diseases. Purpose: The objective of the present work was testing the antileishmanial activity of thioridazine, an antipsychotic agent with demonstrated effect against other intracellular pathogens. Methods: The cytotoxicity for mouse peritoneal macrophages as well as the activity against Leishmania amazonensis, Leishmania mexicana and Leishmania major promastigotes and intracellular amastigotes, as well as in a mouse model of cutaneous leishmaniasis were assessed. Results: Thioridazine inhibited the in vitro proliferation of promastigotes (50 % inhibitory concentration -IC50- values in the range of 0.73 µM to 3.8 µM against L. amazonensis, L. mexicana and L. major) and intracellular amastigotes (IC50 values of 1.27 µM to 4.4 µM for the same species). In contrast, in mouse peritoneal macrophages, the 50 % cytotoxic concentration was 24.0 ± 1.89 µM. Thioridazine inhibited the growth of cutaneous lesions and reduced the number of parasites in the infected tissue of mice. The dose of thioridazine that inhibited lesion development by 50 % compared to controls was 23.3 ± 3.1 mg/kg and in terms of parasite load it was 11.1 ± 0.97 mg/kg. Conclusions: Thioridazine was effective against the promastigote and intracellular amastigote stages of three Leishmania species and in a mouse model of cutaneous leishmaniasis, supporting the potential repurposing of this drug as an antileishmanial agent.

Publisher

Research Square Platform LLC

Reference34 articles.

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