Trypanocidal Activity of Flavanone Derivatives.

Gabriela Maciel Diogo,Policarpo Ademar Sales Junior,Silvane Maria Fonseca Murta,Josimara Souza Andrade,Jason Guy Taylor,Viviane Martins Rebello Dos Santos

doi:10.3390/molecules25020397

Gabriela Maciel Diogo, Policarpo Ademar Sales Junior + Show 4 more

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https://doi.org/10.3390/molecules25020397

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Abstract

Chagas disease, also known as American trypanosomiasis, is classified as a neglected disease by the World Health Organization. For clinical treatment, only two drugs have been on the market, Benznidazole and Nifurtimox, both of which are recommended for use in the acute phase but present low cure rates in the chronic phase. Furthermore, strong side effects may result in discontinuation of this treatment. Faced with this situation, we report the synthesis and trypanocidal activity of 3-benzoyl-flavanones. Novel 3-benzoyl-flavanone derivatives were prepared in satisfactory yields in the 3-step synthetic procedure. According to recommended guidelines, the whole cell-based screening methodology was utilized that allowed for the simultaneous use of both parasite forms responsible for human infection. The majority of the tested compounds displayed promising anti-Trypanosoma cruzi activity and the most potent flavanone bearing a nitrofuran moiety was more potent than the reference drug, Benznidazole.

Highlights

IntroductionThe Brazilian researcher Carlos Ribeiro Justiniano das Chagas discovered Chagas disease ( known as American trypanosomiasis) in 1909 and revealed that the etiologic agent to be the parasiteTrypanosoma cruzi (T. cruzi) [1]
The Brazilian researcher Carlos Ribeiro Justiniano das Chagas discovered Chagas disease in 1909 and revealed that the etiologic agent to be the parasiteTrypanosoma cruzi (T. cruzi) [1]
3-benzoyl-flavanone derivatives 2a–z were synthesized by a domino aldol condensation intramolecular oxi-Michael reaction between β-diketones and aldehydes in the presence of morpholine (Scheme 1)

Summary

Introduction

The Brazilian researcher Carlos Ribeiro Justiniano das Chagas discovered Chagas disease ( known as American trypanosomiasis) in 1909 and revealed that the etiologic agent to be the parasiteTrypanosoma cruzi (T. cruzi) [1]. The Brazilian researcher Carlos Ribeiro Justiniano das Chagas discovered Chagas disease ( known as American trypanosomiasis) in 1909 and revealed that the etiologic agent to be the parasite. Chagas disease is classified by the World Health Organization (WHO). In a recent survey conducted between 2008 and 2017, over 90% of reported cases of Chagas disease in the world were confirmed in South America [5]. A common form of transmission occurs through contact of the mucosa of the open wound with contaminated feces of the triatomine bug [5,6,7]. The transmission is caused by direct contact with the parasite, but it can be caused by indirect contact occurring by ingestion of contaminated food containing feces of the triatomine bug. Studies suggest that the most probable forms of transmission were oral transmission (72%), the minority being caused by vector transmission (9%) and the remaining 19% were unidentified forms of transmission [5]

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