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Plasmodium falciparum: multifaceted resistance to artemisinins.


ABSTRACT: Plasmodium falciparum resistance to artemisinins, the most potent and fastest acting anti-malarials, threatens malaria elimination strategies. Artemisinin resistance is due to mutation of the PfK13 propeller domain and involves an unconventional mechanism based on a quiescence state leading to parasite recrudescence as soon as drug pressure is removed. The enhanced P. falciparum quiescence capacity of artemisinin-resistant parasites results from an increased ability to manage oxidative damage and an altered cell cycle gene regulation within a complex network involving the unfolded protein response, the PI3K/PI3P/AKT pathway, the PfPK4/eIF2? cascade and yet unidentified transcription factor(s), with minimal energetic requirements and fatty acid metabolism maintained in the mitochondrion and apicoplast. The detailed study of these mechanisms offers a way forward for identifying future intervention targets to fend off established artemisinin resistance.

SUBMITTER: Paloque L 

PROVIDER: S-EPMC4784301 | biostudies-other | 2016 Mar

REPOSITORIES: biostudies-other

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Plasmodium falciparum: multifaceted resistance to artemisinins.

Paloque Lucie L   Ramadani Arba P AP   Mercereau-Puijalon Odile O   Augereau Jean-Michel JM   Benoit-Vical Françoise F  

Malaria journal 20160309


Plasmodium falciparum resistance to artemisinins, the most potent and fastest acting anti-malarials, threatens malaria elimination strategies. Artemisinin resistance is due to mutation of the PfK13 propeller domain and involves an unconventional mechanism based on a quiescence state leading to parasite recrudescence as soon as drug pressure is removed. The enhanced P. falciparum quiescence capacity of artemisinin-resistant parasites results from an increased ability to manage oxidative damage an  ...[more]

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