MAINTENANCE EN COURS / SITE UNDER MAINTENANCE

Une opération de maintenance est en cours: les résultats de recherches et les exportations peuvent être incohérent.
Site under maintenance: search & exportation results could be inconsistent.
 

Metabolomics study of 3-O-p-(Z/E)-coumaroyltormentic acid-treated Trypanosoma brucei brucei

Coelho Cristino Mamede, Lucia;Fall, Fanta;Vast, Madeline;Hughes, Kristelle;Leclercq, Joëlle;et.al.
(2025) International journal for parasitology. Drugs and drug resistance — p. 100595 (2025)

Files

2025_Mamede_Int_J_Parasitol_Drugs_Drug_Resist.pdf
  • Open Access
  • Adobe PDF
  • 2.72 MB
  • https://creativecommons.org/licenses/by-nc-nd/4.0/
Download

Details

Authors
  • Coelho Cristino Mamede, Luciaorcid-logoUCLouvain
    Author
  • Fall, FantaUCLouvain
    Author
  • Vast, MadelineUCLouvain
    Author
  • Hughes, Kristelleorcid-logoUCLouvain
    Author
  • Martelli, Giorgiaorcid-logoUCLouvain
    Author
  • Caligiore, Francescoorcid-logoUCLouvain
    Author
  • Govaerts, Bernadetteorcid-logoUCLouvain
    Author
  • Leclercq, Joëlleorcid-logoUCLouvain
    Author
Show more
Abstract
Trypanosomiasis is a parasitic disease for which new treatments are needed due to the frequent occurrence of adverse side effects of current available drugs. Natural compounds found in traditionally used plants offer opportunities to discover innovative compounds that could prove pivotal to antitrypanosomal drug development. 3-O-p-(Z/E)-coumaroyltormentic acids (CTA) were isolated first from the West Africa-native tree Vitellaria paradoxa and have demonstrated quite selective in vitro and in vivo antitrypanosomal activity, despite the unknown mode of action. In this study, a metabolomics analysis using the data from both LC-HR-MS and 1H-NMR described CTA’s effects on Trypanosoma brucei after 3 h exposure under 5 or 10 x EC50. Our study shows CTA’s activity impacted tryptophan metabolism and reveals potential targets in different branches of this metabolism. Our results demonstrate a likely presence of enzymes dedicated to tryptophan, like a tryptophan aminotransferase, tryptophan 2,3-dioxygenase and/or indoleamine 2,3-dioxygenase, and other enzymes of the kynurenine pathway, despite the absence of their description thus far in this species. These data further implicate that CTA’s toxic effect on the tryptophan metabolism may be attributed to the decrease of the intracellular level of essential aspartate, resulting from inhibition of its aminotransferase. In resume, our study shines light on the likelihood of the tryptophan metabolism pathway presenting innovative targets toward the development of antitrypanosomal drugs. These require confirmation through functional and enzymatic studies.
Affiliations

Citations

  • APA
  • Chicago
  • FWB

Coelho Cristino Mamede, L., Fall, F., Vast, M., Hughes, K., Martelli, G., Caligiore, F., Govaerts, B., Michels, P. A. M., Frédérich, M., & Leclercq, J. (2025). Metabolomics study of 3-O-p-(Z/E)-coumaroyltormentic acid-treated Trypanosoma brucei brucei. International journal for parasitology. Drugs and drug resistance, 100595. https://doi.org/10.1016/j.ijpddr.2025.100595 (Original work published 2025)