Prioritization of Molecular Targets for Antimalarial Drug Discovery

Forte, Barbara; Ottilie, Sabine; Plater, Andrew; Campo, Brice; Dechering, Koen J.; Gamo, Francisco Javier; Goldberg, Daniel E.; Istvan, Eva S.; Lee, Marcus; Lukens, Amanda K.; McNamara, Case W.; Niles, Jacquin C.; Okombo, John; Pasaje, Charisse Flerida A.; Siegel, Marvín I.; Wirth, Dyann F.; Wyllie, Susan; Fidock, David A.; Baragaña, Beatriz; Winzeler, Elizabeth A.; Gilbert, Ian H.

doi:10.1021/acsinfecdis.1c00322

Cited by 54 publications

(74 citation statements)

References 58 publications

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“…In future studies it will be interesting to assess precisely to which level FLN-CQ binding contributes to the overall CQ MOA that is known to be intrinsically complex involving multiple molecular factors (see above). Nevertheless, results from this study indicate that the inhibitory CQ binding site on FLN could constitute a promising target for novel antimalaria drugs in the future and put FLN on the list of potential antimalarial drug targets for development programs that are currently ongoing around the world 51,52,[68][69][70] .…”

Section: Discussionmentioning

confidence: 95%

“…Knowledge of drug target(s) is imperative for the development of effective and safe antimalarials. Without knowing which part of the drug interacts with its target, chemical changes needed to improve the compound e cacy and safety are done in a trialerror manner 51,52 . Here, our MS-CETSA based screening approach successfully identi ed a number of potential drug binding partners of CQ and MK-4815 in P. falciparum, with FLN exerting the strongest thermal stabilization.…”

Section: Discussionmentioning

confidence: 99%

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Identification of an inhibitory pocket in falcilysin bound by chloroquine provides a new avenue for malaria drug development

Dziekan

Lin

Sahili

et al. 2022

Preprint

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Despite their widespread use, our understanding of how malaria drugs work remains limited. This includes chloroquine (CQ), the most successful antimalarial ever deployed. Here, we used MS-CETSA and dose-response transcriptional profiling to identify possible protein targets and mechanism of action (MOA) of CQ, as well as MK-4815, a malaria drug candidate with a proposed MOA similar to CQ. Both compounds bind falcilysin (FLN) and hemoglobin digestion was the key biological pathway affected, with distinct MOA profiles between CQ-sensitive and CQ-resistant parasites. We showed that CQ and MK-4815 inhibit FLN proteolytic activity, and using X-ray crystallography, that they occupy a hydrophobic pocket situated within the large peptide substrate binding cavity of FLN. Studies using transgenic parasite line suggest the potential role of FLN in the CQ and MK-4815 MOA. Altogether, our data reveal a druggable pocket in the FLN substrate binding cavity that can be explored in future antimalarial development efforts.

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Section: Discussionmentioning

confidence: 95%

Section: Discussionmentioning

confidence: 99%

Identification of an inhibitory pocket in falcilysin bound by chloroquine provides a new avenue for malaria drug development

Dziekan

Lin

Sahili

et al. 2022

Preprint

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“…The different physiological environment of the target and its binding partners, which are not known, could also account for these differences. Target vulnerability could also play a role; if the parasite is able to survive with low levels of active enzyme, subtle changes in the potency or dissociation rates of inhibitors could affect their in cellulo activity 41 . Alternatively, these compounds could exert their cytotoxic effects through different targets with different mechanisms of action.…”

Section: Groupmentioning

confidence: 99%

“…Our results demonstrate that 45 likely exerts its antiplasmodial activity through inhibition of multiple essential P. falciparum kinases. Polypharmacology has many advantages for antimalarial drug development, as it reduces the likelihood of resistance, provides opportunities for multistage intervention, and may inhibit enzymes of bypass pathways that would otherwise be able to compensate for inhibition of a single target 9,41 .…”

Section: Groupmentioning

confidence: 99%

“…The aqueous layer was extracted with EtOAc (20 mL x 2). The combined organic extracts were washed with water, brine, dried over anhydrous Na2SO4, filtered, concentrated onto Celite, and purified by flash chromatography (40-100% EtOAc in Hexanes on silica gel column) to afford 40 ( (41). To a solution of 4-((4-methylpiperazin-1-yl)methyl)aniline (55 mg, 0.27 mmol, 1.2 eq) in DMSO (1 mL) was added 1,1′carbonyldiimidazole (47 mg, 0.29 mmol, 1.3 eq).…”

Section: -(4-((2-chloropyrimidin-4-yl)oxy)-2-fluorophenyl)-3-(24diflu...mentioning

confidence: 99%

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Discovery of Potent Plasmodium falciparum Protein Kinase 6 (PfPK6) Inhibitors with a Type II Inhibitor Pharmacophore

Ong

Truong

Kwarcinski

et al. 2022

Preprint

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Malaria is a devastating disease that causes significant global morbidity and mortality. The rise of drug resistance against artemisinin-based combination therapy, the frontline treatment for malaria, demonstrates the necessity to develop alternative antimalarials with novel mechanisms of action. Inhibition of Plasmodium protein kinases presents an underexplored opportunity for drug development. PfPK6 has been identified as an essential kinase for P. falciparum asexual blood stage proliferation, but has not been subjected to medicinal chemistry campaigns for inhibitor development. In this work, we report the discovery of Ki8751 as a PfPK6 inhibitor (IC50 = 14 nM) determined using the KinaseSeeker assay, utilizing split-luciferase three-hybrid technology. A series of 79 1-phenyl-3-(4-(quinolin-4-yloxy)phenyl)urea derivatives of Ki8751 were designed, synthesized and evaluated for PfPK6 inhibition and antiplasmodial activity. Using group efficiency analyses, we established the importance of the key groups on the scaffold for inhibition of PfPK6 consistent with a type II inhibitor pharmacophore. We highlight modifications on the tail group that contribute to antiplasmodial activity. We report the discovery of compound 67, a potent PfPK6 inhibitor (IC50 = 13 nM) active against the P. falciparum blood stage (EC50 = 160 nM), and compound 79, an excellent PfPK6 inhibitor (IC50 < 5 nM) with dual-stage antiplasmodial activity against P. falciparum blood stage (EC50 = 39 nM) and against P. berghei liver stage (EC50 = 220 nM). These results lay the foundation for this chemotype to be further developed into novel antimalarials and into chemical probes targeting PfPK6, enabling further investigation into PfPK6 function.

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Substrate Peptidomimetic Inhibitors of P. falciparum Plasmepsin X with Potent Antimalarial Activity

et al. 2022

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Plasmepsin X (PMX) is an aspartyl protease that processes proteins essential for Plasmodium parasites to invade and egress from host erythrocytes during the symptomatic asexual stage of malaria. PMX substrates possess a conserved cleavage region denoted by the consensus motif, SFhE (h=hydrophobic amino acid). Peptidomimetics reflecting the P3‐P1 positions of the consensus motif were designed and showed potent and selective inhibition of PMX. It was established that PMX prefers Phe in the P1 position, di‐substitution at the β‐carbon of the P2 moiety and a hydrophobic P3 group which was supported by modelling of the peptidomimetics in complex with PMX. The peptidomimetics were shown to arrest asexual P. falciparum parasites at the schizont stage by impairing PMX substrate processing. Overall, the peptidomimetics described will assist in further understanding PMX substrate specificity and have the potential to act as a template for future antimalarial design.

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Prioritization of Molecular Targets for Antimalarial Drug Discovery

Cited by 54 publications

References 58 publications

Identification of an inhibitory pocket in falcilysin bound by chloroquine provides a new avenue for malaria drug development

Identification of an inhibitory pocket in falcilysin bound by chloroquine provides a new avenue for malaria drug development

Discovery of Potent Plasmodium falciparum Protein Kinase 6 (PfPK6) Inhibitors with a Type II Inhibitor Pharmacophore

Substrate Peptidomimetic Inhibitors of P. falciparum Plasmepsin X with Potent Antimalarial Activity

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