Richard K. Haynes scite author profile

Artemisinin—the next generation: Efficacies of artemisone against the malaria parasite are substantially greater than those of the current artemisinin “gold standard”, artesunate. Also, in contrast to most current artemisinins it displays low lipophilicity and negligible neuro‐ and cytotoxicity in in vitro and in vivo assays. Thus, the drug offers promise for use in artemisinin‐based combination therapy.

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A single amino acid residue can determine the sensitivity of SERCAs to artemisinins

Uhlemann

Cameron

Eckstein-Ludwig

et al. 2005

Nat Struct Mol Biol

231

210

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Artemisinins are the most important class of antimalarial drugs. They specifically inhibit PfATP6, a SERCA-type ATPase of Plasmodium falciparum. Here we show that a single amino acid in transmembrane segment 3 of SERCAs can determine susceptibility to artemisinin. An L263E replacement of a malarial by a mammalian residue abolishes inhibition by artemisinins. Introducing residues found in other Plasmodium spp. also modulates artemisinin sensitivity, suggesting that artemisinins interact with the thapsigargin-binding cleft of susceptible SERCAs.

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Artemisinins: their growing importance in medicine

Krishna

Bustamante

Haynes

et al. 2008

Trends in Pharmacological Sciences

322

186

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Artemisinins are derived from extracts of sweet wormwood (Artemisia annua) and are well established for the treatment of malaria, including highly drug-resistant strains. Their efficacy also extends to phylogenetically unrelated parasitic infections such as schistosomiasis. More recently, they have also shown potent and broad anticancer properties in cell lines and animal models. In this review, we discuss recent advances in defining the role of artemisinins in medicine, with particular focus on their controversial mechanisms of action. This safe and cheap drug class that saves lives at risk from malaria can also have important potential in oncology.

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Richard K. Haynes

Artemisone—A Highly Active Antimalarial Drug of the Artemisinin Class

A single amino acid residue can determine the sensitivity of SERCAs to artemisinins

Artemisinins: their growing importance in medicine

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