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Review
. 2021 Dec 21;12(6):e0242521.
doi: 10.1128/mBio.02425-21. Epub 2021 Nov 16.

Bacterial Approaches for Assembling Iron-Sulfur Proteins

Karla Esquilin-Lebron  1 Sarah Dubrac  2 Frédéric Barras  2 Jeffrey M Boyd  1
Affiliations
Review

Bacterial Approaches for Assembling Iron-Sulfur Proteins

Karla Esquilin-Lebron et al. mBio. .

Abstract

Building iron-sulfur (Fe-S) clusters and assembling Fe-S proteins are essential actions for life on Earth. The three processes that sustain life, photosynthesis, nitrogen fixation, and respiration, require Fe-S proteins. Genes coding for Fe-S proteins can be found in nearly every sequenced genome. Fe-S proteins have a wide variety of functions, and therefore, defective assembly of Fe-S proteins results in cell death or global metabolic defects. Compared to alternative essential cellular processes, there is less known about Fe-S cluster synthesis and Fe-S protein maturation. Moreover, new factors involved in Fe-S protein assembly continue to be discovered. These facts highlight the growing need to develop a deeper biological understanding of Fe-S cluster synthesis, holo-protein maturation, and Fe-S cluster repair. Here, we outline bacterial strategies used to assemble Fe-S proteins and the genetic regulation of these processes. We focus on recent and relevant findings and discuss future directions, including the proposal of using Fe-S protein assembly as an antipathogen target.

Keywords: ISC; NIF; SUF; bacteria; genetic regulation; iron; iron regulation; iron utilization; iron-sulfur cluster; metalloproteins; metalloregulation; sulfide; sulfur.

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Figures

FIG 1
FIG 1
General mechanism of bacterial Fe-S protein assembly. Monoatomic Fe2+ and S0 are combined with electrons on a proteinaceous molecular scaffold forming an Fe-S cluster. The Fe-S cluster is transferred to one or more carrier proteins before being transferred to an apo-protein forming a holo-protein. Reactive oxygen species (ROS) can either damage the Fe-S cluster, which can subsequently be repaired, or destroy it, resulting in apo-protein formation.
FIG 2
FIG 2
Iron-sulfur cluster synthesis. (A) Structure of IscU from Thermus thermophilus (PDB accession number 2QQ4). The gray ball is a Zn(II) ion, and the side chains of the three ligating cysteines are highlighted. (B) Structure of SufBC2D from Escherichia coli (PDB accession number 5AWF). SufC is shown in green, and SufB and SufD are shown in purple and tan, respectively. (C) Working models for ISC- and SUF-directed iron-sulfur protein maturation in Escherichia coli.
FIG 3
FIG 3
Iron-sulfur cluster carriage. (A) Structure of the A-type carrier IscA from Thermosynechococcus elongatus (PDB accession number 1X0G) with a [2Fe-2S] cluster bound. (B) Structure of Nfu from Staphylococcus epidermidis (PDB accession number 1XHJ). The cysteine thiols that are proposed iron-sulfur cluster ligands are highlighted. (C) Schematic representation of iron-sulfur cluster scaffolds and carriers.
FIG 4
FIG 4
Regulation of iron-sulfur cluster synthesis in Escherichia coli. (A) X-ray structure of an apo-IscR monomer with the proposed Fe-S cluster ligands (C92A, C98A, C104A, and H107) highlighted in red (PDB accession number 4HF1). Note that in this IscR variant, the ligating cysteines have been changed to alanines. (B) X-ray structure of dimeric apo-IscR bound to the hya promoter, which is a type 2 binding site (PDB accession number 4HF1). Each monomer is differently colored (blue and pink). (C) Model for the regulation of ISC and SUF expression in Escherichia coli.
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