| Literature DB >> 31987792 |
Anais Laleve1, Cristina Panozzo2, Inge Kühl2, Alexa Bourand-Plantefol2, Jelena Ostojic2, Abdoulaye Sissoko3, Déborah Tribouillard-Tanvier4, David Cornu2, Angélique Burg2, Brigitte Meunier2, Marc Blondel4, Jerome Clain3, Nathalie Bonnefoy2, Romain Duval3, Geneviève Dujardin5.
Abstract
Artemisinin and its derivatives kill malaria parasites and inhibit the proliferation of cancer cells. In both processes, heme was shown to play a key role in artemisinin bioactivation. We found that artemisinin and clinical artemisinin derivatives are able to compensate for a mutation in the yeast Bcs1 protein, a key chaperon involved in biogenesis of the mitochondrial respiratory complex III. The equivalent Bcs1 variant causes an encephalopathy in human by affecting complex III assembly. We show that artemisinin derivatives decrease the content of mitochondrial cytochromes and disturb the maturation of the complex III cytochrome c1. This last effect is likely responsible for the compensation by decreasing the detrimental over-accumulation of the inactive pre-complex III observed in the bcs1 mutant. We further show that a fluorescent dihydroartemisinin probe rapidly accumulates in the mitochondrial network and targets cytochromes c and c1 in yeast, human cells and isolated mitochondria. In vitro this probe interacts with purified cytochrome c only under reducing conditions and we detect cytochrome c-dihydroartemisinin covalent adducts by mass spectrometry analyses. We propose that reduced mitochondrial c-type cytochromes act as both targets and mediators of artemisinin bioactivation in yeast and human cells.Entities:
Keywords: Artemisinins; Bcs1; Fluorescent probe; Mitochondria; c-Type cytochromes
Year: 2020 PMID: 31987792 DOI: 10.1016/j.bbamcr.2020.118661
Source DB: PubMed Journal: Biochim Biophys Acta Mol Cell Res ISSN: 0167-4889 Impact factor: 4.739