Issue 7, 2024

Novel flexible biphenyl PfDHFR inhibitors with improved antimalarial activity

Abstract

As pregnant women and young children remain the first victims of malaria worldwide, the search for new antimalarials has been focusing on compounds with a high safety profile and extended efficacy. In a previous study, a rigid biphenyl PfDHFR inhibitor was developed by fragment-based screening, displaying sub nM enzyme inhibition but poor antiparasitic activity, presumably due to its low flexibility. Here, we report a new series of compounds that combines the biphenyl fragment with a flexible linker. Interestingly, their mode of binding differs from previously reported compounds, taking advantage of strong hydrophobic interaction. The new flexible biphenyl compounds show overall improved antiparasitic activity compared to rigid ones, with the best compound displaying a 2 nM antiplasmodial IC50 and suitable drug-like properties. This confirms the importance of compound flexibility for antimalarial activity and opens the way to new opportunities for antimalarial drug design.

Graphical abstract: Novel flexible biphenyl PfDHFR inhibitors with improved antimalarial activity

Supplementary files

Article information

Article type
Research Article
Submitted
22 Mar 2024
Accepted
09 May 2024
First published
30 May 2024

RSC Med. Chem., 2024,15, 2496-2507

Novel flexible biphenyl PfDHFR inhibitors with improved antimalarial activity

S. Decharuangsilp, U. Arwon, N. Sooksai, R. Rattanajak, T. Saeyang, D. Vitsupakorn, J. Vanichtanankul, Y. Yuthavong, S. Kamchonwongpaisan and M. Hoarau, RSC Med. Chem., 2024, 15, 2496 DOI: 10.1039/D4MD00197D

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