Interaction between diterpene icetexanes and old yellow enzymes of Leishmania braziliensis and Trypanosoma cruzi

Old Yellow Enzymes (OYEs) are flavin-dependent redox enzymes that promote the asymmetric reduction of activated alkenes. Due to the high importance of flavoenzymes in the metabolism of organisms, the interaction between OYEs from the parasites Trypanosoma cruzi and Leishmania braziliensis and three...

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Veröffentlicht in:International journal of biological macromolecules 2024-02, Vol.259 (Pt 2), p.129192-129192, Article 129192
Hauptverfasser: Libardi, Silvia H., Ahmad, Anees, Ferreira, Francis B., Oliveira, Ronaldo J., Caruso, Ícaro P., Melo, Fernando A., de Albuquerque, Sergio, Cardoso, Daniel R., Burtoloso, Antonio C.B., Borges, Júlio C.
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container_end_page 129192
container_issue Pt 2
container_start_page 129192
container_title International journal of biological macromolecules
container_volume 259
creator Libardi, Silvia H.
Ahmad, Anees
Ferreira, Francis B.
Oliveira, Ronaldo J.
Caruso, Ícaro P.
Melo, Fernando A.
de Albuquerque, Sergio
Cardoso, Daniel R.
Burtoloso, Antonio C.B.
Borges, Júlio C.
description Old Yellow Enzymes (OYEs) are flavin-dependent redox enzymes that promote the asymmetric reduction of activated alkenes. Due to the high importance of flavoenzymes in the metabolism of organisms, the interaction between OYEs from the parasites Trypanosoma cruzi and Leishmania braziliensis and three diterpene icetexanes (brussonol and two analogs), were evaluated in the present study, and differences in the binding mechanism and inhibition capacity of these molecules were examined. Although the aforementioned compounds showed poor and negligible activities against T. cruzi and L. braziliensis cells, respectively, the experiments with the purified enzymes indicated that the interaction occurs by divergent mechanisms. Overall, the ligands' inhibitory effect depends on their accessibility to the N5 position of the flavin's isoalloxazine ring. The results also indicated that the OYEs found in both parasites share structural similarities and showed affinities for the diterpene icetexanes in the same range. Nevertheless, the interaction between OYEs and ligands is directed by enthalpy and/or entropy in distinct ways. In conclusion, the binding site of both OYEs exhibits remarkable plasticity, and a large range of different molecules, including that can be substrates and inhibitors, can bind this site. This plasticity should be considered in drug design using OYE as a target.
doi_str_mv 10.1016/j.ijbiomac.2023.129192
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Due to the high importance of flavoenzymes in the metabolism of organisms, the interaction between OYEs from the parasites Trypanosoma cruzi and Leishmania braziliensis and three diterpene icetexanes (brussonol and two analogs), were evaluated in the present study, and differences in the binding mechanism and inhibition capacity of these molecules were examined. Although the aforementioned compounds showed poor and negligible activities against T. cruzi and L. braziliensis cells, respectively, the experiments with the purified enzymes indicated that the interaction occurs by divergent mechanisms. Overall, the ligands' inhibitory effect depends on their accessibility to the N5 position of the flavin's isoalloxazine ring. The results also indicated that the OYEs found in both parasites share structural similarities and showed affinities for the diterpene icetexanes in the same range. Nevertheless, the interaction between OYEs and ligands is directed by enthalpy and/or entropy in distinct ways. In conclusion, the binding site of both OYEs exhibits remarkable plasticity, and a large range of different molecules, including that can be substrates and inhibitors, can bind this site. 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subjects Chagas Disease - parasitology
Flavins - pharmacology
Humans
Leishmania braziliensis
Ligand binding
NADPH Dehydrogenase - chemistry
NADPH Dehydrogenase - pharmacology
Neglected diseases
OYEs
Protozoa
Trypanosoma cruzi
title Interaction between diterpene icetexanes and old yellow enzymes of Leishmania braziliensis and Trypanosoma cruzi
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