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Targeted Inhibition of Plasmodium falciparum Calcium-Dependent Protein Kinase 1 with a Constrained J Domain-Derived Disruptor Peptide



Details zur Publikation
Autor(inn)en:
Flaherty, B.; Ho, T.; Schmidt, S.; Herberg, F.; Peterson, D.; Kennedy, E.

Publikationsjahr:
2019
Zeitschrift:
ACS infectious diseases
Seitenbereich:
506-514
Jahrgang/Band :
5
Heftnummer:
4
DOI-Link der Erstveröffentlichung:


Zusammenfassung, Abstract
To explore the possibility of constrained peptides to target Plasmodium-infected cells, we designed a J domain mimetic derived from Plasmodium falciparum calcium-dependent protein kinase 1 ( PfCDPK1) as a strategy to disrupt J domain binding and inhibit PfCDPK1 activity. The J domain disruptor (JDD) peptide was conformationally constrained using a hydrocarbon staple and was found to selectively permeate segmented schizonts and colocalize with intracellular merozoites in late-stage parasites. In vitro analyses demonstrated that JDD could effectively inhibit the catalytic activity of recombinant PfCDPK1 in the low micromolar range. Treatment of late-stage parasites with JDD resulted in a significant decrease in parasite viability mediated by a blockage of merozoite invasion, consistent with a primary effect of PfCDPK1 inhibition. To the best of our knowledge, this marks the first use of stapled peptides designed to specifically target a Plasmodium falciparum protein and demonstrates that stapled peptides may serve as useful tools for exploring potential antimalarial agents.


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Zuletzt aktualisiert 2023-02-06 um 18:59