Recent Advances in the Development of Triose Phosphate Isomerase Inhibitors as Antiprotozoal Agents

Lenci K Vázquez-Jiménez; Antonio Moreno-Herrera; Alfredo Juárez-Saldivar; Alonzo González-González; Eyra Ortiz-Pérez; Alma D Paz-González; Isidro Palos; Esther Ramírez-Moreno; Gildardo Rivera

doi:10.2174/0929867328666210913090928

Recent Advances in the Development of Triose Phosphate Isomerase Inhibitors as Antiprotozoal Agents

Curr Med Chem. 2022;29(14):2504-2529. doi: 10.2174/0929867328666210913090928.

Authors

Lenci K Vázquez-Jiménez¹, Antonio Moreno-Herrera¹, Alfredo Juárez-Saldivar¹, Alonzo González-González¹, Eyra Ortiz-Pérez¹, Alma D Paz-González¹, Isidro Palos², Esther Ramírez-Moreno³, Gildardo Rivera¹

Affiliations

¹ Laboratorio de Biotecnología Farmacéutica, Centro de Biotecnología Genómica, Instituto Politécnico Nacional, 88710 Reynosa, México.
² Unidad Académica Multidisciplinaria Reynosa-Rodhe, Universidad Autónoma de Tamaulipas, 88779 Reynosa, México.
³ Escuela Nacional de Medicina y Homeopatía, Instituto Politécnico Nacional, 07320 Ciudad de México, México.

PMID: 34517794
DOI: 10.2174/0929867328666210913090928

Abstract

Background: Parasitic diseases caused by protozoa, such as Chagas disease, leishmaniasis, malaria, African trypanosomiasis, amoebiasis, trichomoniasis, and giardiasis, are considered serious public health problems in developing countries. Drug resistance among parasites justifies the search for new therapeutic drugs, and the identification of new targets becomes a valuable approach. In this scenario, the glycolysis pathway, which converts glucose into pyruvate, plays an important role in the protozoa energy supply, and it is therefore considered a promising target. In this pathway, triose phosphate isomerase (TIM) plays an essential role in efficient energy production. Furthermore, protozoa TIM shows structural differences with human enzyme counterparts, suggesting the possibility of obtaining selective inhibitors. Therefore, TIM is considered a valid approach to develop new antiprotozoal agents, inhibiting the glycolysis in the parasite.

Objective: In this review, we discuss the drug design strategies, structure-activity relationship, and binding modes of outstanding TIM inhibitors against Trypanosoma cruzi, Trypanosoma brucei, Plasmodium falciparum, Giardia lamblia, Leishmania mexicana, Trichomonas vaginalis, and Entamoeba histolytica.

Results: TIM inhibitors have mainly shown aromatic systems and symmetrical structure, where the size and type of heteroatom are important for enzyme inhibition. This inhibition is mainly based on the interaction with i) the interfacial region of TIM inducing changes on the quaternary and tertiary structure or ii) with the TIM catalytic region, the main pathways that disable the catalytic activity of the enzyme.

Conclusion: Benzothiazole, benzoxazole, benzimidazole, and sulfhydryl derivatives stand out as TIM inhibitors. In silico and in vitro studies have demonstrated that the inhibitors bind mainly at the TIM dimer interface. In this review, the development of new TIM inhibitors as antiprotozoal drugs is demonstrated as an important pharmaceutical strategy that may lead to new therapies for these ancient parasitic diseases.

Keywords: Antiprotozoal; drugs; inhibitors; molecular docking; parasitic diseases; triose phosphate isomerase.

Publication types

Review

MeSH terms

Antiprotozoal Agents* / chemistry
Antiprotozoal Agents* / pharmacology
Antiprotozoal Agents* / therapeutic use
Chagas Disease* / drug therapy
Humans
Triose-Phosphate Isomerase / chemistry
Triose-Phosphate Isomerase / metabolism
Trypanosoma brucei brucei*
Trypanosoma cruzi*

Substances

Antiprotozoal Agents
Triose-Phosphate Isomerase

Grants and funding

SIP-20210050/Secretaria de Investigacion y Posgrado del Instituto Politecnico Nacional