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Export Malaria continues to pose a significant health threat, causing thousands of deaths each year. The limited availability of vaccines and medications, combined with the emergence of drug resistance, further complicates the fight against this disease. In this study, we aimed to enhance the antimalarial potency of the previously reported hit compound BIPPO (pIC(50) 5.9). Through systematic modification of pyrazolopyrimidinone analogs, we discovered the promising analog 30 (NPD-3547), which exhibited approximately one log unit higher in vitro potency (pIC(50) 6.8) against Plasmodium falciparum. Furthermore, we identified several other BIPPO analogs (23, 28, 29 and 47a) with potent antimalarial activity (pIC(50) > 6.0) and favorable metabolic stability in mouse liver microsomes. These compounds can serve as new tools for further optimization towards the development of potential candidates for antimalarial studies.
SEEK ID: https://fairdomhub.org/publications/731
PubMed ID: 37446602
Projects: WG1 - Compound libraries coordination and integration of compound design, WG2 - Integration of early phase studies and low environmental impact ac..., WG3 - Coordination of in vitro-to-in vivo translation of OneHealth leads..., WG4 - Integration of R&D process-environmental studies and translation i...
Publication type: Journal Article
Journal: Molecules
Citation: Molecules. 2023 Jun 23;28(13):4939. doi: 10.3390/molecules28134939.
Date Published: 23rd Jun 2023
Registered Mode: by PubMed ID
SubmitterViews: 13
Created: 13th Jul 2026 at 13:04
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https://orcid.org/0000-0002-4870-3202