Stabilisation of the RirA [4Fe–4S] cluster results in loss of iron-sensing function

RirA is a global iron regulator in diverse Alphaproteobacteria that belongs to the Rrf2 superfamily of transcriptional regulators, which can contain an iron–sulfur (Fe–S) cluster. Under iron-replete conditions, RirA contains a [4Fe–4S] cluster, enabling high-affinity binding to RirA-regulated operat...

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Autores principales: Gray, Elizabeth, Stewart, Melissa Y. Y., Hanwell, Libby, Crack, Jason C., Devine, Rebecca, Stevenson, Clare E. M., Volbeda, Anne, Johnston, Andrew W. B., Fontecilla-Camps, Juan C., Hutchings, Matthew I., Todd, Jonathan D., Le Brun, Nick E.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: The Royal Society of Chemistry 2023
Materias:
Chemistry
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10510648/
https://www.ncbi.nlm.nih.gov/pubmed/37736639
http://dx.doi.org/10.1039/d3sc03020b
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author Gray, Elizabeth
Stewart, Melissa Y. Y.
Hanwell, Libby
Crack, Jason C.
Devine, Rebecca
Stevenson, Clare E. M.
Volbeda, Anne
Johnston, Andrew W. B.
Fontecilla-Camps, Juan C.
Hutchings, Matthew I.
Todd, Jonathan D.
Le Brun, Nick E.
author_facet Gray, Elizabeth
Stewart, Melissa Y. Y.
Hanwell, Libby
Crack, Jason C.
Devine, Rebecca
Stevenson, Clare E. M.
Volbeda, Anne
Johnston, Andrew W. B.
Fontecilla-Camps, Juan C.
Hutchings, Matthew I.
Todd, Jonathan D.
Le Brun, Nick E.
author_sort Gray, Elizabeth
collection PubMed
description RirA is a global iron regulator in diverse Alphaproteobacteria that belongs to the Rrf2 superfamily of transcriptional regulators, which can contain an iron–sulfur (Fe–S) cluster. Under iron-replete conditions, RirA contains a [4Fe–4S] cluster, enabling high-affinity binding to RirA-regulated operator sequences, thereby causing the repression of cellular iron uptake. Under iron deficiency, one of the cluster irons dissociates, generating an unstable [3Fe–4S] form that subsequently degrades to a [2Fe–2S] form and then to apo RirA, resulting in loss of high-affinity DNA-binding. The cluster is coordinated by three conserved cysteine residues and an unknown fourth ligand. Considering the lability of one of the irons and the resulting cluster fragility, we hypothesized that the fourth ligand may not be an amino acid residue. To investigate this, we considered that the introduction of an amino acid residue that could coordinate the cluster might stabilize it. A structural model of RirA, based on the Rrf2 family nitrosative stress response regulator NsrR, highlighted residue 8, an Asn in the RirA sequence, as being appropriately positioned to coordinate the cluster. Substitution of Asn8 with Asp, the equivalent, cluster-coordinating residue of NsrR, or with Cys, resulted in proteins that contained a [4Fe–4S] cluster, with N8D RirA exhibiting spectroscopic properties very similar to NsrR. The variant proteins retained the ability to bind RirA-regulated DNA, and could still act as repressors of RirA-regulated genes in vivo. However, they were significantly more stable than wild-type RirA when exposed to O(2) and/or low iron. Importantly, they exhibited reduced capacity to respond to cellular iron levels, even abolished in the case of the N8D version, and thus were no longer iron sensing. This work demonstrates the importance of cluster fragility for the iron-sensing function of RirA, and more broadly, how a single residue substitution can alter cluster coordination and functional properties in the Rrf2 superfamily of regulators.
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spelling pubmed-105106482023-09-21 Stabilisation of the RirA [4Fe–4S] cluster results in loss of iron-sensing function Gray, Elizabeth Stewart, Melissa Y. Y. Hanwell, Libby Crack, Jason C. Devine, Rebecca Stevenson, Clare E. M. Volbeda, Anne Johnston, Andrew W. B. Fontecilla-Camps, Juan C. Hutchings, Matthew I. Todd, Jonathan D. Le Brun, Nick E. Chem Sci Chemistry RirA is a global iron regulator in diverse Alphaproteobacteria that belongs to the Rrf2 superfamily of transcriptional regulators, which can contain an iron–sulfur (Fe–S) cluster. Under iron-replete conditions, RirA contains a [4Fe–4S] cluster, enabling high-affinity binding to RirA-regulated operator sequences, thereby causing the repression of cellular iron uptake. Under iron deficiency, one of the cluster irons dissociates, generating an unstable [3Fe–4S] form that subsequently degrades to a [2Fe–2S] form and then to apo RirA, resulting in loss of high-affinity DNA-binding. The cluster is coordinated by three conserved cysteine residues and an unknown fourth ligand. Considering the lability of one of the irons and the resulting cluster fragility, we hypothesized that the fourth ligand may not be an amino acid residue. To investigate this, we considered that the introduction of an amino acid residue that could coordinate the cluster might stabilize it. A structural model of RirA, based on the Rrf2 family nitrosative stress response regulator NsrR, highlighted residue 8, an Asn in the RirA sequence, as being appropriately positioned to coordinate the cluster. Substitution of Asn8 with Asp, the equivalent, cluster-coordinating residue of NsrR, or with Cys, resulted in proteins that contained a [4Fe–4S] cluster, with N8D RirA exhibiting spectroscopic properties very similar to NsrR. The variant proteins retained the ability to bind RirA-regulated DNA, and could still act as repressors of RirA-regulated genes in vivo. However, they were significantly more stable than wild-type RirA when exposed to O(2) and/or low iron. Importantly, they exhibited reduced capacity to respond to cellular iron levels, even abolished in the case of the N8D version, and thus were no longer iron sensing. This work demonstrates the importance of cluster fragility for the iron-sensing function of RirA, and more broadly, how a single residue substitution can alter cluster coordination and functional properties in the Rrf2 superfamily of regulators. The Royal Society of Chemistry 2023-08-22 /pmc/articles/PMC10510648/ /pubmed/37736639 http://dx.doi.org/10.1039/d3sc03020b Text en This journal is © The Royal Society of Chemistry https://creativecommons.org/licenses/by/3.0/
spellingShingle Chemistry
Gray, Elizabeth
Stewart, Melissa Y. Y.
Hanwell, Libby
Crack, Jason C.
Devine, Rebecca
Stevenson, Clare E. M.
Volbeda, Anne
Johnston, Andrew W. B.
Fontecilla-Camps, Juan C.
Hutchings, Matthew I.
Todd, Jonathan D.
Le Brun, Nick E.
Stabilisation of the RirA [4Fe–4S] cluster results in loss of iron-sensing function
title Stabilisation of the RirA [4Fe–4S] cluster results in loss of iron-sensing function
title_full Stabilisation of the RirA [4Fe–4S] cluster results in loss of iron-sensing function
title_fullStr Stabilisation of the RirA [4Fe–4S] cluster results in loss of iron-sensing function
title_full_unstemmed Stabilisation of the RirA [4Fe–4S] cluster results in loss of iron-sensing function
title_short Stabilisation of the RirA [4Fe–4S] cluster results in loss of iron-sensing function
title_sort stabilisation of the rira [4fe–4s] cluster results in loss of iron-sensing function
topic Chemistry
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10510648/
https://www.ncbi.nlm.nih.gov/pubmed/37736639
http://dx.doi.org/10.1039/d3sc03020b
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