Litcius/Paper detail

The newly discovered role of endocytosis in artemisinin resistance

Hannah Michaela Behrens, Sabine Schmidt, Tobias Spielmann

2021Medicinal Research Reviews32 citationsDOIOpen Access PDF

Abstract

Artemisinin and its derivatives (ART) are the cornerstone of malaria treatment as part of artemisinin combination therapy (ACT). However, reduced susceptibility to artemisinin as well as its partner drugs threatens the usefulness of ACTs. Single point mutations in the parasite protein Kelch13 (K13) are necessary and sufficient for the reduced sensitivity of malaria parasites to ART but several alternative mechanisms for this resistance have been proposed. Recent work found that K13 is involved in the endocytosis of host cell cytosol and indicated that this is the process responsible for resistance in parasites with mutated K13. These studies also identified a series of further proteins that act together with K13 in the same pathway, including previously suspected resistance proteins such as UBP1 and AP-2μ. Here, we give a brief overview of artemisinin resistance, present the recent evidence of the role of endocytosis in ART resistance and discuss previous hypotheses in light of this new evidence. We also give an outlook on how the new insights might affect future research.

Topics & Concepts

ArtemisininEndocytosisPharmacologyBiologyMedicineChemistryMalariaReceptorImmunologyPlasmodium falciparumGeneticsMalaria Research and ControlTrypanosoma species research and implicationsMosquito-borne diseases and control