Identification of Chalcones as Fasciola hepatica Cathepsin L Inhibitors Using a Comprehensive Experimental and Computational Approach

Florencia Ferraro; Alicia Merlino; Nicolás Dell Oca; Jorge Gil; José F Tort; Mercedes Gonzalez; Hugo Cerecetto; Mauricio Cabrera; Ileana Corvo

doi:10.1371/journal.pntd.0004834

Identification of Chalcones as Fasciola hepatica Cathepsin L Inhibitors Using a Comprehensive Experimental and Computational Approach

PLoS Negl Trop Dis. 2016 Jul 27;10(7):e0004834. doi: 10.1371/journal.pntd.0004834. eCollection 2016 Jul.

Authors

Florencia Ferraro^{1

2}, Alicia Merlino², Nicolás Dell Oca³, Jorge Gil⁴, José F Tort³, Mercedes Gonzalez⁵, Hugo Cerecetto^{5

6}, Mauricio Cabrera^{1

5}, Ileana Corvo^{1

3}

Affiliations

¹ Laboratorio de Investigación y Desarrollo de Moléculas Bioactivas, Departamento de Ciencias Biológicas, CENUR Litoral Norte, Universidad de la República, Paysandú, Uruguay.
² Laboratorio de Química Teórica y Computacional, Instituto de Química Biológica, Facultad de Ciencias, Universidad de la República, Montevideo, Uruguay.
³ Departamento de Genética, Facultad de Medicina, Universidad de la República, Montevideo, Uruguay.
⁴ Laboratorio de Reproducción Animal, Producción y Reproducción de Rumiantes, Departamento de Ciencias Biológicas, CENUR Litoral Norte-Facultad de Veterinaria, Universidad de la República, Paysandú, Uruguay.
⁵ Grupo de Química Medicinal, Laboratorio de Química Orgánica, Facultad de Ciencias, Universidad de la República, Montevideo, Uruguay.
⁶ Área de Radiofarmacia, Centro de Investigaciones Nucleares, Facultad de Ciencias, Universidad de la República, Montevideo, Uruguay.

Abstract

Background: Increased reports of human infections have led fasciolosis, a widespread disease of cattle and sheep caused by the liver flukes Fasciola hepatica and Fasciola gigantica, to be considered an emerging zoonotic disease. Chemotherapy is the main control measure available, and triclabendazole is the preferred drug since is effective against both juvenile and mature parasites. However, resistance to triclabendazole has been reported in several countries urging the search of new chemical entities and target molecules to control fluke infections.

Methodology/principle findings: We searched a library of forty flavonoid derivatives for inhibitors of key stage specific Fasciola hepatica cysteine proteases (FhCL3 and FhCL1). Chalcones substituted with phenyl and naphtyl groups emerged as good cathepsin L inhibitors, interacting more frequently with two putative binding sites within the active site cleft of the enzymes. One of the compounds, C34, tightly bounds to juvenile specific FhCL3 with an IC50 of 5.6 μM. We demonstrated that C34 is a slow-reversible inhibitor that interacts with the Cys-His catalytic dyad and key S2 and S3 pocket residues, determinants of the substrate specificity of this family of cysteine proteases. Interestingly, C34 induces a reduction in NEJ ability to migrate through the gut wall and a loss of motility phenotype that leads to NEJ death within a week in vitro, while it is not cytotoxic to bovine cells.

Conclusions/significance: Up to date there are no reports of in vitro screening for non-peptidic inhibitors of Fasciola hepatica cathepsins, while in general these are considered as the best strategy for in vivo inhibition. We have identified chalcones as novel inhibitors of the two main Cathepsins secreted by juvenile and adult liver flukes. Interestingly, one compound (C34) is highly active towards the juvenile enzyme reducing larval ability to penetrate the gut wall and decreasing NEJ´s viability in vitro. These findings open new avenues for the development of novel agents to control fluke infection and possibly other helminthic diseases.

Publication types

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

MeSH terms

Animals
Cathepsin L / antagonists & inhibitors*
Cathepsin L / metabolism
Chalcones / chemistry
Chalcones / pharmacology*
Computer Simulation
Fasciola hepatica / metabolism*
Models, Biological
Models, Molecular
Molecular Structure
Protein Conformation
Recombinant Proteins

Substances

Chalcones
Recombinant Proteins
Cathepsin L

Grants and funding

This work was partially funded by Programa de Desarrollo de las Ciencias Básicas (www.pedeciba.edu.uy) and Agencia Nacional de Investigación e Innovación (www.anii.org.uy) granted an scolarship INI_X_2013_1_100964 to FF. The funders had no role in study design, data collection and analysis, decision to publish, or preparation of the manuscript.