1. Academic Validation
  2. Identification of Innovative Folate Inhibitors Leveraging the Amino Dihydrotriazine Motif from Cycloguanil for Their Potential as Anti- Trypanosoma brucei Agents

Identification of Innovative Folate Inhibitors Leveraging the Amino Dihydrotriazine Motif from Cycloguanil for Their Potential as Anti- Trypanosoma brucei Agents

  • ACS Infect Dis. 2024 Jul 2. doi: 10.1021/acsinfecdis.4c00113.
Valeria Francesconi 1 Marco Rizzo 1 Cecilia Pozzi 2 3 Lorenzo Tagliazucchi 4 5 Claude U Konchie Simo 4 Giulia Saporito 4 Giacomo Landi 2 Stefano Mangani 2 Anna Carbone 1 Silvia Schenone 1 Nuno Santarém 6 Joana Tavares 6 Anabela Cordeiro-da-Silva 6 7 Maria Paola Costi 4 Michele Tonelli 1
Affiliations

Affiliations

  • 1 Department of Pharmacy, University of Genoa, viale Benedetto XV n.3, Genoa 16132, Italy.
  • 2 Department of Biotechnology, Chemistry and Pharmacy, University of Siena, via Aldo Moro 2, Siena 53100, Italy.
  • 3 Consorzio Interuniversitario Risonanze Magnetiche di Metallo Proteine (CIMMP), Via Luigi Sacconi 6, Sesto Fiorentino (FI) 50019, Italy.
  • 4 Department of Life Science, University of Modena and Reggio Emilia, via Campi 103, Modena 41125, Italy.
  • 5 Doctorate School in Clinical and Experimental Medicine (CEM), University of Modena and Reggio Emilia, Via Campi 287, Modena 41125, Italy.
  • 6 i3S - Institute for Research and Innovation in Health, University of Porto, Rua Alfredo Allen, 208, Porto 4200-135, Portugal.
  • 7 Department of Life Science, Faculty of Pharmacy, University of Porto, Rua de Jorge Viterbo Ferreira, 228, Porto 4050-313, Portugal.
Abstract

Folate Enzymes, namely, dihydrofolate reductase (DHFR) and pteridine reductase (PTR1) are acknowledged targets for the development of antiparasitic agents against Trypanosomiasis and Leishmaniasis. Based on the amino dihydrotriazine motif of the drug Cycloguanil (Cyc), a known inhibitor of both folate Enzymes, we have identified two novel series of inhibitors, the 2-amino triazino benzimidazoles (1) and 2-guanidino benzimidazoles (2), as their open ring analogues. Enzymatic screening was carried out against PTR1, DHFR, and Thymidylate Synthase (TS). The crystal structures of TbDHFR and TbPTR1 in complex with selected compounds experienced in both cases a substrate-like binding mode and allowed the rationalization of the main chemical features supporting the inhibitor ability to target folate Enzymes. Biological evaluation of both series was performed against T. brucei and L. infantum and the toxicity against THP-1 human macrophages. Notably, the 5,6-dimethyl-2-guanidinobenzimidazole 2g resulted to be the most potent (Ki = 9 nM) and highly selective TbDHFR inhibitor, 6000-fold over TbPTR1 and 394-fold over hDHFR. The 5,6-dimethyl tricyclic analogue 1g, despite showing a lower potency and selectivity profile than 2g, shared a comparable antiparasitic activity against T. brucei in the low micromolar domain. The dichloro-substituted 2-guanidino benzimidazoles 2c and 2d revealed their potent and broad-spectrum antitrypanosomatid activity affecting the growth of T. brucei and L. infantum parasites. Therefore, both chemotypes could represent promising templates that could be valorized for further drug development.

Keywords

Leishmania infantum; Trypanosoma brucei; antiparasitic agents; dihydrofolate reductase inhibitors; pteridine reductase inhibitors; triazino and guanidino benzimidazoles.

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