The indole motif is essential for the antitrypanosomal activity of N5-substituted paullones

Ihnatenko, Irina; Müller, Marco J.; Orban, Oliver C. F.; Lindhof, Jens C.; Benítez, Diego; Ortíz, Cecilia; Dibello, Estefanía; Seidl, Leonardo L.; Comini, Marcelo A.; Kunick, Conrad

doi:10.1371/journal.pone.0292946

Cited by 2 publications

(1 citation statement)

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“…Several of the new derivatives showed good inhibitory properties behaving as uncompetitive enzyme inhibitors and resulted in improved potency and selectivity against L. braziliensis and L. infantum [148]. Recently, it has been reported that the indole moiety of N 5 -substituted paullones is essential for keeping the TryS-inhibitory and antitrypanosomal activity of this type of compound [149].…”

Section: Substrate or Transition State Analogsmentioning

confidence: 99%

Targeting Trypanothione Metabolism in Trypanosomatids

González-Montero,

Andrés-Rodríguez,

García-Fernández

et al. 2024

Molecules

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Infectious diseases caused by trypanosomatids, including African trypanosomiasis (sleeping sickness), Chagas disease, and different forms of leishmaniasis, are Neglected Tropical Diseases affecting millions of people worldwide, mainly in vulnerable territories of tropical and subtropical areas. In general, current treatments against these diseases are old-fashioned, showing adverse effects and loss of efficacy due to misuse or overuse, thus leading to the emergence of resistance. For these reasons, searching for new antitrypanosomatid drugs has become an urgent necessity, and different metabolic pathways have been studied as potential drug targets against these parasites. Considering that trypanosomatids possess a unique redox pathway based on the trypanothione molecule absent in the mammalian host, the key enzymes involved in trypanothione metabolism, trypanothione reductase and trypanothione synthetase, have been studied in detail as druggable targets. In this review, we summarize some of the recent findings on the molecules inhibiting these two essential enzymes for Trypanosoma and Leishmania viability.

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Section: Substrate or Transition State Analogsmentioning

confidence: 99%

Targeting Trypanothione Metabolism in Trypanosomatids

González-Montero,

Andrés-Rodríguez,

García-Fernández

et al. 2024

Molecules

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Expanding the applications of a bioluminescent mouse infection model of acute African trypanosomiasis

Benítez,

Ortíz,

Dibello

et al. 2024

Front. Chem. Biol.

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IntroductionIn vivo imaging technology based on bioluminescence has contributed to the study of different pathophysiological conditions involving inherited or transmissible diseases. Here, we aimed to establish a bioluminescent model of acute African trypanosomiasis for a manifold of applications. African trypanosomiasis is a neglected tropical disease that threatens human and animal health, mainly in sub-Saharan countries, for which new chemotherapies are needed.MethodsThe model relies on a hypervirulent bloodstream form of Trypanosoma brucei brucei, which constitutively expresses red-shifted luciferase, and an infection-susceptible murine host, Balb/cJ mouse. In vivo and ex vivo imaging techniques were applied to obtain a spatial, temporal, and quantitative (parasite load) resolution of the infection process and to refine the animal endpoint criterion.ResultsThe model proved suitable for validating the essentiality of the parasite enzyme glucose 6-phosphate dehydrogenase by reverse genetics (tetracycline-inducible double-strand RNA interference). The efficacy of drugs (monotherapy or a new combination) for the treatment of the acute stage of the disease was successfully explored by in vivo imaging.DiscussionThe new bioluminescent model developed here may represent a valuable tool for speeding up the drug discovery process and the investigation of host-pathogen interactions in the acute stage of African sleeping sickness.

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The indole motif is essential for the antitrypanosomal activity of N5-substituted paullones

Cited by 2 publications

References 74 publications

Targeting Trypanothione Metabolism in Trypanosomatids

Targeting Trypanothione Metabolism in Trypanosomatids

Expanding the applications of a bioluminescent mouse infection model of acute African trypanosomiasis

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