Repurpose antimalarials to target Toxoplasma gondii dihydrofolate reductase thymidylate synthase

Decharuangsilp S.; Koompapong K.; Arwon U.; Tuyapala N.; Hoarau M.; Tanasugarn L.; Pengon J.; Talawanich Y.; Saeyang T.; Vanichtanankul J.; Yuthavong Y.; Kamchonwongpaisan S.; Mahittikorn A.; Kongkasuriyachai D.

Repurpose antimalarials to target Toxoplasma gondii dihydrofolate reductase thymidylate synthase

Issued Date

2026-09-05

Resource Type

Article

ISSN

02235234

eISSN

17683254

DOI

10.1016/j.ejmech.2026.118863

Scopus ID

2-s2.0-105037073717

Journal Title

European Journal of Medicinal Chemistry

Volume

313

Rights Holder(s)

SCOPUS

Bibliographic Citation

European Journal of Medicinal Chemistry Vol.313 (2026)

Suggested Citation

Decharuangsilp S., Koompapong K., Arwon U., Tuyapala N., Hoarau M., Tanasugarn L., Pengon J., Talawanich Y., Saeyang T., Vanichtanankul J., Yuthavong Y., Kamchonwongpaisan S., Mahittikorn A., Kongkasuriyachai D. Repurpose antimalarials to target Toxoplasma gondii dihydrofolate reductase thymidylate synthase. European Journal of Medicinal Chemistry Vol.313 (2026). doi:10.1016/j.ejmech.2026.118863 Retrieved from: https://repository.li.mahidol.ac.th/handle/123456789/116515

Title

Repurpose antimalarials to target Toxoplasma gondii dihydrofolate reductase thymidylate synthase

Author(s)

Decharuangsilp S.
Koompapong K.
Arwon U.
Tuyapala N.
Hoarau M.
Tanasugarn L.
Pengon J.
Talawanich Y.
Saeyang T.
Vanichtanankul J.
Yuthavong Y.
Kamchonwongpaisan S.
Mahittikorn A.
Kongkasuriyachai D.

Author's Affiliation

Faculty of Tropical Medicine, Mahidol University
Thailand National Center for Genetic Engineering and Biotechnology
Thailand National Nanotechnology Center

Corresponding Author(s)

Decharuangsilp S.

Other Contributor(s)

Mahidol University

Abstract

Toxoplasma gondii is an obligate intracellular blood and tissue protozoan parasite that infects up to a third of the population worldwide. Several antimalarial drugs, in particular pyrimethamine (PYR), have been used for decades to treat toxoplasmosis. Here, the clinical candidate P218, a potent inhibitor of Plasmodium falciparum dihydrofolate reductase (PfDHFR), and a series of flexible diaminopyrimidine butyrolactone analogues were identified as potent T. gondii dihydrofolate reductase (TgDHFR) inhibitors. The most promising butyrolactone analogue, LA4, displayed an improved TgDHFR inhibition (K<inf>i</inf> 1.71 nM), increased antiparasitic properties in vitro (IC<inf>50</inf> 0.44 nM), and a higher cell selectivity compared to PYR (K<inf>i</inf> 13.0 nM, IC<inf>50</inf> 410 nM) while P218 (K<inf>i</inf> 2.19 nM, IC<inf>50</inf> 370 nM) presented an improved activity with comparable cell selectivity to PYR. The in vivo results against T. gondii RH strain-infected mice showed that P218 reduced parasitic burden in blood whereas LA4 decreased parasite load in peritoneal fluid and blood with an extended mice survival. These findings position butyrolactone LA4 as a new potential for the treatment of acute toxoplasmosis.

Keyword(s)

Pharmacology, Toxicology and Pharmaceutics
Chemistry

URI

https://repository.li.mahidol.ac.th/handle/123456789/116515

Collections

Scopus 2026

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