Parasite Metalo-aminopeptidases as Targets in Human Infectious Diseases

Mirtha E Aguado; Maikel Izquierdo; Maikel González-Matos; Ana C Varela; Yanira Méndez; Maday A Del Rivero; Daniel G Rivera; Jorge González-Bacerio

doi:10.2174/1389450124666230224140724

Parasite Metalo-aminopeptidases as Targets in Human Infectious Diseases

Curr Drug Targets. 2023;24(5):416-461. doi: 10.2174/1389450124666230224140724.

Authors

Mirtha E Aguado¹, Maikel Izquierdo¹, Maikel González-Matos¹, Ana C Varela¹, Yanira Méndez², Maday A Del Rivero¹, Daniel G Rivera², Jorge González-Bacerio^{1

3}

Affiliations

¹ Center for Protein Studies, Faculty of Biology, University of Havana, Calle 25 #455 Entre I y J, 10400, Vedado, La Habana, Cuba.
² Center for Natural Products Research, Faculty of Chemistry, University of Havana, Zapata y G, 10400, La Habana, Cuba.
³ Department of Biochemistry, Faculty of Biology, University of Havana, calle 25 #455 entre I y J, 10400, Vedado, La Habana, Cuba.

PMID: 36825701
DOI: 10.2174/1389450124666230224140724

Abstract

Background: Parasitic human infectious diseases are a worldwide health problem due to the increased resistance to conventional drugs. For this reason, the identification of novel molecular targets and the discovery of new chemotherapeutic agents are urgently required. Metalo- aminopeptidases are promising targets in parasitic infections. They participate in crucial processes for parasite growth and pathogenesis.

Objective: In this review, we describe the structural, functional and kinetic properties, and inhibitors, of several parasite metalo-aminopeptidases, for their use as targets in parasitic diseases.

Conclusion: Plasmodium falciparum M1 and M17 aminopeptidases are essential enzymes for parasite development, and M18 aminopeptidase could be involved in hemoglobin digestion and erythrocyte invasion and egression. Trypanosoma cruzi, T. brucei and Leishmania major acidic M17 aminopeptidases can play a nutritional role. T. brucei basic M17 aminopeptidase down-regulation delays the cytokinesis. The inhibition of Leishmania basic M17 aminopeptidase could affect parasite viability. L. donovani methionyl aminopeptidase inhibition prevents apoptosis but not the parasite death. Decrease in Acanthamoeba castellanii M17 aminopeptidase activity produces cell wall structural modifications and encystation inhibition. Inhibition of Babesia bovis growth is probably related to the inhibition of the parasite M17 aminopeptidase, probably involved in host hemoglobin degradation. Schistosoma mansoni M17 aminopeptidases inhibition may affect parasite development, since they could participate in hemoglobin degradation, surface membrane remodeling and eggs hatching. Toxoplasma gondii M17 aminopeptidase inhibition could attenuate parasite virulence, since it is apparently involved in the hydrolysis of cathepsin Cs- or proteasome-produced dipeptides and/or cell attachment/invasion processes. These data are relevant to validate these enzymes as targets.

Keywords: Antiparasite agents; divalent metal cations; enzyme-inhibitor complexes; metalo-aminopeptidases; pathogenic parasites; protease inhibitors.

Publication types

Review

MeSH terms

Aminopeptidases
Animals
Communicable Diseases*
Humans
Parasites* / metabolism
Plasmodium falciparum
Toxoplasma*

Substances

Aminopeptidases

Grants and funding

GLACIER 57592717 for DGR and JGB/Cuban Heritage Collection