ATM1, an essential conserved transporter in Apicomplexa, bridges mitochondrial and cytosolic [Fe-S] biogenesis

生物 生物发生 顶复亚门 线粒体 胞浆 运输机 恶性疟原虫 细胞生物学 线粒体生物发生 铁硫簇 生物化学 基因 疟疾 免疫学
作者
D. L. Shrivastava,Ernest Abboud,Jadhav Prasad Ramchandra,A. Jha,Jean‐Baptiste Marq,Animesh Chaurasia,Kalyan Mitra,Mohammad Sadik,Mohammad Imran Siddiqi,Dominique Soldati‐Favre,Joachim Kloehn,Saman Habib
出处
期刊:PLOS Pathogens [Public Library of Science]
卷期号:20 (9): e1012593-e1012593
标识
DOI:10.1371/journal.ppat.1012593
摘要

The Apicomplexa phylum encompasses numerous obligate intracellular parasites, some associated with severe implications for human health, including Plasmodium , Cryptosporidium , and Toxoplasma gondii . The iron-sulfur cluster [Fe-S] biogenesis ISC pathway, localized within the mitochondrion or mitosome of these parasites, is vital for parasite survival and development. Previous work on T . gondii and Plasmodium falciparum provided insights into the mechanisms of [Fe-S] biogenesis within this phylum, while the transporter linking mitochondria-generated [Fe-S] with the cytosolic [Fe-S] assembly (CIA) pathway remained elusive. This critical step is catalyzed by a well-conserved ABC transporter, termed ATM1 in yeast, ATM3 in plants and ABCB7 in mammals. Here, we identify and characterize this transporter in two clinically relevant Apicomplexa. We demonstrate that depletion of Tg ATM1 does not specifically impair mitochondrial metabolism. Instead, proteomic analyses reveal that Tg ATM1 expression levels inversely correlate with the abundance of proteins that participate in the transfer of [Fe-S] to cytosolic proteins at the outer mitochondrial membrane. Further insights into the role of Tg ATM1 are gained through functional complementation with the well-characterized yeast homolog. Biochemical characterization of Pf ATM1 confirms its role as a functional ABC transporter, modulated by oxidized glutathione (GSSG) and [4Fe-4S].
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