Literature DB >> 26099175

The role of mitochondria and the CIA machinery in the maturation of cytosolic and nuclear iron-sulfur proteins.

Roland Lill1, Rafal Dutkiewicz2, Sven A Freibert3, Torsten Heidenreich4, Judita Mascarenhas3, Daili J Netz4, Viktoria D Paul4, Antonio J Pierik5, Nadine Richter4, Martin Stümpfig4, Vasundara Srinivasan3, Oliver Stehling4, Ulrich Mühlenhoff4.   

Abstract

Mitochondria have been derived from alpha-bacterial endosymbionts during the evolution of eukaryotes. Numerous bacterial functions have been maintained inside the organelles including fatty acid degradation, citric acid cycle, oxidative phosphorylation, and the synthesis of heme or lipoic acid cofactors. Additionally, mitochondria have inherited the bacterial iron-sulfur cluster assembly (ISC) machinery. Many of the ISC components are essential for cell viability because they generate a still unknown, sulfur-containing compound for the assembly of cytosolic and nuclear Fe/S proteins that perform important functions in, e.g., protein translation, DNA synthesis and repair, and chromosome segregation. The sulfur-containing compound is exported by the mitochondrial ABC transporter Atm1 (human ABCB7) and utilized by components of the cytosolic iron-sulfur protein assembly (CIA) machinery. An appealing minimal model for the striking compartmentation of eukaryotic Fe/S protein biogenesis is provided by organisms that contain mitosomes instead of mitochondria. Mitosomes have been derived from mitochondria by reductive evolution, during which they have lost virtually all classical mitochondrial tasks. Nevertheless, mitosomes harbor all core ISC components which presumably have been maintained for assisting the maturation of cytosolic-nuclear Fe/S proteins. The current review is centered around the Atm1 export process. We present an overview on the mitochondrial requirements for the export reaction, summarize recent insights into the 3D structure and potential mechanism of Atm1, and explain how the CIA machinery uses the mitochondrial export product for the assembly of cytosolic and nuclear Fe/S proteins.
Copyright © 2015 Elsevier GmbH. All rights reserved.

Entities:  

Keywords:  ABC transporter; Atm1–ABCB7; Cysteine desulfurase; Frataxin; Glutaredoxin; Glutathione; Iron storage disease; Iron–sulfur cluster; Membrane transport

Mesh:

Substances:

Year:  2015        PMID: 26099175     DOI: 10.1016/j.ejcb.2015.05.002

Source DB:  PubMed          Journal:  Eur J Cell Biol        ISSN: 0171-9335            Impact factor:   4.492


  71 in total

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