Energy metabolism as a target for cyclobenzaprine: A drug candidate against Visceral Leishmaniasis

Marta Lopes Lima; Maria A Abengózar; Eduardo Caio Torres-Santos; Samanta Etel Treiger Borborema; Joanna Godzien; Ángeles López-Gonzálvez; Coral Barbas; Luis Rivas; Andre Gustavo Tempone

doi:10.1016/j.bioorg.2022.106009

Energy metabolism as a target for cyclobenzaprine: A drug candidate against Visceral Leishmaniasis

Bioorg Chem. 2022 Oct:127:106009. doi: 10.1016/j.bioorg.2022.106009. Epub 2022 Jul 6.

Authors

Marta Lopes Lima¹, Maria A Abengózar², Eduardo Caio Torres-Santos³, Samanta Etel Treiger Borborema¹, Joanna Godzien⁴, Ángeles López-Gonzálvez⁴, Coral Barbas⁵, Luis Rivas⁶, Andre Gustavo Tempone⁷

Affiliations

¹ Centre for Parasitology and Mycology, Instituto Adolfo Lutz, São Paulo, São Paulo, Brazil.
² Centro de Investigaciones Biológicas Margarita Salas (CSIC), Madrid, Spain.
³ Laboratório de Bioquímica de Tripanosomatídeos, Instituto Oswaldo Cruz, Fiocruz, Rio de Janeiro, Brazil.
⁴ Centre for Metabolomics and Bioanalysis (CEMBIO), Faculty of Pharmacy, Universidad CEU San Pablo, Madrid, Spain.
⁵ Centre for Metabolomics and Bioanalysis (CEMBIO), Faculty of Pharmacy, Universidad CEU San Pablo, Madrid, Spain. Electronic address: cbarbas@ceu.es.
⁶ Centro de Investigaciones Biológicas Margarita Salas (CSIC), Madrid, Spain. Electronic address: luis.rivas@cib.csic.es.
⁷ Centre for Parasitology and Mycology, Instituto Adolfo Lutz, São Paulo, São Paulo, Brazil. Electronic address: andre.tempone@ial.sp.gov.br.

PMID: 35841672
DOI: 10.1016/j.bioorg.2022.106009

Abstract

Leishmaniases have a broad spectrum of clinical manifestations, ranging from a cutaneous to a progressive and fatal visceral disease. Chemotherapy is nowadays the almost exclusive way to fight the disease but limited by its scarce therapeutic arsenal, on its own compromised by adverse side effects and clinical resistance. Cyclobenzaprine (CBP), an FDA-approved oral muscle relaxant drug has previously demonstrated in vitro and in vivo activity against Leishmania sp., but its targets were not fully unveiled. This study aimed to define the role of energy metabolism as a target for the leishmanicidal mechanisms of CBP. Methodology to assess CBP leishmanicidal mechanism variation of intracellular ATP levels using living Leishmania transfected with a cytoplasmic luciferase. Induction of plasma membrane permeability by assessing depolarization with DiSBAC(2)3 and entrance of the vital dye SYTOX® Green. Mitochondrial depolarization by rhodamine 123 accumulation. Mapping target site within the respiratory chain by oxygen consumption rate. Reactive oxygen species (ROS) production using MitoSOX. Morphological changes by transmission electron microscopy. CBP caused on L. infantum promastigotes a decrease of intracellular ATP levels, with irreversible depolarization of plasma membrane, the collapse of the mitochondrial electrochemical potential, mild uncoupling of the respiratory chain, and ROS production, with ensuing intracellular Ca²⁺ imbalance and DNA fragmentation. Electron microscopy supported autophagic features but not a massive plasma membrane disruption. The severe and irreversible mitochondrial damage induced by CBP endorsed the bioenergetics metabolism as a relevant target within the lethal programme induced by CBP in Leishmania. This, together with the mild-side effects of this oral drug, endorses CBP as an appealing novel candidate as a leishmanicidal drug under a drug repurposing strategy.

Keywords: Cyclobenzaprine; Drug repurposing; Leishmania; Leishmaniasis; Mechanism of action; Neglected diseases.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Adenosine Triphosphate / metabolism
Amitriptyline / analogs & derivatives
Animals
Antiprotozoal Agents* / metabolism
Energy Metabolism
Humans
Leishmania infantum*
Leishmaniasis, Visceral* / drug therapy
Mice
Mice, Inbred BALB C
Reactive Oxygen Species / metabolism

Substances

Antiprotozoal Agents
Reactive Oxygen Species
Amitriptyline
cyclobenzaprine
Adenosine Triphosphate