Histidinal-based potent antimalarial agents

TitleHistidinal-based potent antimalarial agents
Publication TypeJournal Article
Year of Publication2023
AuthorsMeena, CL, Hingamire, T, Gupta, T, Deshmukh, B, Karmodiya, K, Joshi, R, Shanmugam, D, Sanjayan, GJ
JournalChemMedChem
Volume18
Issue9
Date PublishedMAY
Type of ArticleArticle
ISSN1860-7179
Keywordsartemisinin, chloroquine, digestive vacuole, docking, falcipains, falciparum, P
Abstract

Herein we report the synthesis and evaluation of peptide-histidinal conjugated drug scaffolds, which have the potential to target the hemoglobin-degrading proteases falcipain-2/3 from the human malaria parasite. Scaffolds with various substitutions were tested for antimalarial activity, and compounds 8 g, 8 h, and 15 exhibited EC50 values of similar to 0.018 mu M, similar to 0.069 mu M, and similar to 0.02 mu M, respectively. Structure-based docking studies on falcipain-2/3 proteases (PDB:2GHU and PDB:3BWK) revealed that compounds 8 g, 8 h, and 15 interact strongly with binding sites of falcipain-2/3 in a substrate-like manner. In silico ADME studies revealed that the molecules of interest showed no or minimal violations of drug-likeness parameters. Further, phenotypic assays revealed that compound 8 g and its biotinylated version inhibit hemoglobin degradation in the parasite food vacuole. The identification of falcipain-2/3 targeting potent inhibitors of the malaria parasite can serve as a starting point for the development of lead compounds as future antimalarial drug candidates.

DOI10.1002/cmdc.202200709
Type of Journal (Indian or Foreign)

Foreign

Impact Factor (IF)

3.540

Divison category: 
Biochemical Sciences
Organic Chemistry
Database: 
Web of Science (WoS)

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