Lactam Truncation Yields a Dihydroquinazolinone Scaffold with Potent Antimalarial Activity that Targets PfATP4.

Trent D Ashton ORCID logo ; Petar PS Calic ORCID logo ; Madeline G Dans ORCID logo ; Zi Kang Ooi ; Qingmiao Zhou ; Katie Loi ORCID logo ; Kate E Jarman ORCID logo ; Josephine Palandri ; Deyun Qiu ORCID logo ; Adele M Lehane ORCID logo ; +14 more... Bikash Maity ; Nirupam De ; Mufuliat T Famodimu ORCID logo ; Michael J Delves ORCID logo ; Emma Y Mao ORCID logo ; Maria R Gancheva ORCID logo ; Danny W Wilson ORCID logo ; Mrittika Chowdury ; Tania F de Koning-Ward ; Delphine Baud ; Stephen Brand ; Paul F Jackson ; Alan F Cowman ORCID logo ; Brad E Sleebs ORCID logo ; (2024) Lactam Truncation Yields a Dihydroquinazolinone Scaffold with Potent Antimalarial Activity that Targets PfATP4. ChemMedChem, 19 (24). e202400549-. ISSN 1860-7179 DOI: 10.1002/cmdc.202400549
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The emergence of resistance against current antimalarial treatments has necessitated the need for the development of novel antimalarial chemotypes. Toward this goal, we recently optimised the antimalarial activity of the dihydroquinazolinone scaffold and showed it targeted PfATP4. Here, we deconstruct the lactam moiety of the tricyclic dihydroquinazolinone scaffold and investigate the structure-activity relationship of the truncated scaffold. It was shown that SAR between scaffolds was largely transferrable and generated analogues with potent asexual stage activity. Evaluation of the truncated analogues against PfATP4 mutant drug-resistant parasite strains and in assays measuring PfATP4-associated ATPase activity demonstrated retention of PfATP4 as the molecular target. Analogues exhibited activity against both male and female gametes and multidrug resistant parasites. Limited efficacy of analogues in a P. berghei asexual stage mouse model was attributed to their moderate metabolic stability and low aqueous stability. Further development is required to address these attributes toward the potential use of the dihydroquinazolinone class in a curative and transmission blocking combination antimalarial therapy.


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