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1. Plasmodium falciparum protein phosphatase PP7 is required for early ring-stage development.

2. Mixed alkyl/aryl phosphonates identify metabolic serine hydrolases as antimalarial targets.

3. The malaria parasite egress protease SUB1 is activated through precise, plasmepsin X-mediated cleavage of the SUB1 prodomain.

4. Peptidic Boronic Acid Plasmodium falciparum SUB1 Inhibitors with Improved Selectivity over Human Proteasome.

5. Activation loop phosphorylation and cGMP saturation of PKG regulate egress of malaria parasites.

6. Mixed Alkyl/Aryl Phosphonates Identify Metabolic Serine Hydrolases as Antimalarial Targets.

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