Literature DB >> 18366324

Maturation of iron-sulfur proteins in eukaryotes: mechanisms, connected processes, and diseases.

Roland Lill1, Ulrich Mühlenhoff.   

Abstract

Iron-sulfur (Fe/S) proteins are involved in a wide variety of cellular processes such as enzymatic reactions, respiration, cofactor biosynthesis, ribosome biogenesis, regulation of gene expression, and DNA-RNA metabolism. Assembly of Fe/S clusters, small inorganic cofactors, is assisted by complex proteinaceous machineries, which use cysteine as a source of sulfur, combine it with iron to synthesize an Fe/S cluster on scaffold proteins, and finally incorporate the cluster into recipient apoproteins. In eukaryotes, such as yeast and human cells, more than 20 components are known that facilitate the maturation of Fe/S proteins in mitochondria, cytosol, and nucleus. These biogenesis components also perform crucial roles in other cellular pathways, e.g., in the regulation of iron homeostasis or the modification of tRNA. Numerous diseases including several neurodegenerative and hematological disorders have been associated with defects in Fe/S protein biogenesis, underlining the central importance of this process for life.

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Year:  2008        PMID: 18366324     DOI: 10.1146/annurev.biochem.76.052705.162653

Source DB:  PubMed          Journal:  Annu Rev Biochem        ISSN: 0066-4154            Impact factor:   23.643


  255 in total

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4.  Mutation in the Fe-S scaffold protein Isu bypasses frataxin deletion.

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Review 9.  Assembly of nonheme Mn/Fe active sites in heterodinuclear metalloproteins.

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10.  Regulation of mitochondrial iron import through differential turnover of mitoferrin 1 and mitoferrin 2.

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