Pyrimidine Azepine Targets the Plasmodium bc1 Complex and Displays Multistage Antimalarial Activity

Juliana Calit, Surendra K. Prajapati, Ernest D. Benavente, Jessica E. Araújo, Bingbing Deng, Kazutoyo Miura, Yasmin Annunciato, Igor M.R. Moura, Miho Usui, Jansen F. Medeiros, Carolina H. Andrade, Sabrina Silva-Mendonca, Anton Simeonov, Richard T. Eastman, Carole A. Long, Maisa da Silva Araujo, Kim C. Williamson, Anna Caroline C. Aguiar*, Daniel Y. Bargieri*

*Corresponding author for this work

Research output: Contribution to journalArticleAcademicpeer-review

Abstract

Malaria control and elimination efforts would benefit from the identification and validation of new malaria chemotherapeutics. Recently, a transgenic Plasmodium berghei line was used to perform a series of high-throughput in vitro screens for new antimalarials acting against the parasite sexual stages. The screens identified pyrimidine azepine chemotypes with potent activity. Here, we validate the activity of PyAz90, the most potent pyrimidine azepine chemotype identified, against P. falciparum and P. vivax in the asexual and sexual stages. PyAz90 blocked parasite transmission to the mosquito vector at nanomolar concentrations and inhibited in vitro asexual parasite multiplication with a fast-action profile. Through the generation of P. falciparum PyAz90-resistant parasites and in vitro assays of mitochondrial activity, we identified cytochrome b as a molecular target of PyAz90. This work characterizes a promising chemotype that can be explored for the future development of new antimalarials targeting the Plasmodium cytochrome bc1 complex.

Original languageEnglish
Number of pages11
JournalJACS Au
Volume4
Issue number10
Early online date7 Oct 2024
DOIs
Publication statusPublished - 28 Oct 2024

Keywords

  • bc complex
  • malaria
  • Plasmodium
  • pyrimidine azepine
  • resistance

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