Mitochondrial [2Fe‐2S] ferredoxins: new functions for old dogs

Author:

Schulz Vinzent12,Freibert Sven‐A.12,Boss Linda12,Mühlenhoff Ulrich12,Stehling Oliver12,Lill Roland12ORCID

Affiliation:

1. Institut für Zytobiologie Philipps‐Universität Marburg Germany

2. Zentrum für Synthetische Mikrobiologie Synmikro Marburg Germany

Abstract

Ferredoxins (FDXs) comprise a large family of iron–sulfur proteins that shuttle electrons from NADPH and FDX reductases into diverse biological processes. This review focuses on the structure, function and specificity of mitochondrial [2Fe‐2S] FDXs that are related to bacterial FDXs due to their endosymbiotic inheritance. Their classical function in cytochrome P450‐dependent steroid transformations was identified around 1960, and is exemplified by mammalian FDX1 (aka adrenodoxin). Thirty years later the essential function in cellular Fe/S protein biogenesis was discovered for the yeast mitochondrial FDX Yah1 that is additionally crucial for the formation of haem a and ubiquinone CoQ6. In mammals, Fe/S protein biogenesis is exclusively performed by the FDX1 paralog FDX2, despite the high structural similarity of both proteins. Recently, additional and specific roles of human FDX1 in haem a and lipoyl cofactor biosyntheses were described. For lipoyl synthesis, FDX1 transfers electrons to the radical S‐adenosyl methionine‐dependent lipoyl synthase to kickstart its radical chain reaction. The high target specificity of the two mammalian FDXs is contained within small conserved sequence motifs, that upon swapping change the target selection of these electron donors.

Funder

Deutsche Forschungsgemeinschaft

Volkswagen Foundation

Publisher

Wiley

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