Human mitochondrial ferritin improves respiratory function in yeast mutants deficient in iron–sulfur cluster biogenesis, but is not a functional homologue of yeast frataxin

We overexpressed human mitochondrial ferritin in frataxin-deficient yeast cells (Δyfh1), but also in another mutant affected in [Fe-S] assembly (Δggc1). Ferritin was correctly processed and expressed in the mitochondria of these cells, but the fraction of total mitochondrial iron bound to ferritin w...

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Autores principales: Sutak, Robert, Seguin, Alexandra, Garcia-Serres, Ricardo, Oddou, Jean-Louis, Dancis, Andrew, Tachezy, Jan, Latour, Jean-Marc, Camadro, Jean-Michel, Lesuisse, Emmanuel
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Blackwell Publishing Inc 2012
Materias:
Original Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3426411/
https://www.ncbi.nlm.nih.gov/pubmed/22950017
http://dx.doi.org/10.1002/mbo3.18
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author Sutak, Robert
Seguin, Alexandra
Garcia-Serres, Ricardo
Oddou, Jean-Louis
Dancis, Andrew
Tachezy, Jan
Latour, Jean-Marc
Camadro, Jean-Michel
Lesuisse, Emmanuel
author_facet Sutak, Robert
Seguin, Alexandra
Garcia-Serres, Ricardo
Oddou, Jean-Louis
Dancis, Andrew
Tachezy, Jan
Latour, Jean-Marc
Camadro, Jean-Michel
Lesuisse, Emmanuel
author_sort Sutak, Robert
collection PubMed
description We overexpressed human mitochondrial ferritin in frataxin-deficient yeast cells (Δyfh1), but also in another mutant affected in [Fe-S] assembly (Δggc1). Ferritin was correctly processed and expressed in the mitochondria of these cells, but the fraction of total mitochondrial iron bound to ferritin was very low, and most of the iron remained in the form of insoluble particles of ferric phosphate in these mitochondria, as evidenced by gel filtration analysis of the mitochondrial matrix (fast protein liquid chromatography [FPLC]) and by Mössbauer spectroscopy. Mutant cells in which ferritin was overexpressed still accumulated iron in the mitochondria and remained deficient in [Fe-S] assembly, suggesting that human mitochondrial ferritin is not a functional homologue of yeast frataxin. However, the respiratory function was improved in these mutants, which correlates with an improvement of cytochrome and heme synthesis. Overexpression of mitochondrial ferritin in [Fe-S] mutants resulted in the appearance of a small pool of high-spin ferrous iron in the mitochondria, which was probably responsible for the improvement of heme synthesis and of the respiratory function in these mutants.
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spelling pubmed-34264112012-08-29 Human mitochondrial ferritin improves respiratory function in yeast mutants deficient in iron–sulfur cluster biogenesis, but is not a functional homologue of yeast frataxin Sutak, Robert Seguin, Alexandra Garcia-Serres, Ricardo Oddou, Jean-Louis Dancis, Andrew Tachezy, Jan Latour, Jean-Marc Camadro, Jean-Michel Lesuisse, Emmanuel Microbiologyopen Original Research We overexpressed human mitochondrial ferritin in frataxin-deficient yeast cells (Δyfh1), but also in another mutant affected in [Fe-S] assembly (Δggc1). Ferritin was correctly processed and expressed in the mitochondria of these cells, but the fraction of total mitochondrial iron bound to ferritin was very low, and most of the iron remained in the form of insoluble particles of ferric phosphate in these mitochondria, as evidenced by gel filtration analysis of the mitochondrial matrix (fast protein liquid chromatography [FPLC]) and by Mössbauer spectroscopy. Mutant cells in which ferritin was overexpressed still accumulated iron in the mitochondria and remained deficient in [Fe-S] assembly, suggesting that human mitochondrial ferritin is not a functional homologue of yeast frataxin. However, the respiratory function was improved in these mutants, which correlates with an improvement of cytochrome and heme synthesis. Overexpression of mitochondrial ferritin in [Fe-S] mutants resulted in the appearance of a small pool of high-spin ferrous iron in the mitochondria, which was probably responsible for the improvement of heme synthesis and of the respiratory function in these mutants. Blackwell Publishing Inc 2012-06 /pmc/articles/PMC3426411/ /pubmed/22950017 http://dx.doi.org/10.1002/mbo3.18 Text en © 2012 The Authors. Published by Blackwell Publishing Ltd. http://creativecommons.org/licenses/by/2.5/ This is an open access article under the terms of the Creative Commons Attribution Non Commercial License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited and is not used for commercial purposes.
spellingShingle Original Research
Sutak, Robert
Seguin, Alexandra
Garcia-Serres, Ricardo
Oddou, Jean-Louis
Dancis, Andrew
Tachezy, Jan
Latour, Jean-Marc
Camadro, Jean-Michel
Lesuisse, Emmanuel
Human mitochondrial ferritin improves respiratory function in yeast mutants deficient in iron–sulfur cluster biogenesis, but is not a functional homologue of yeast frataxin
title Human mitochondrial ferritin improves respiratory function in yeast mutants deficient in iron–sulfur cluster biogenesis, but is not a functional homologue of yeast frataxin
title_full Human mitochondrial ferritin improves respiratory function in yeast mutants deficient in iron–sulfur cluster biogenesis, but is not a functional homologue of yeast frataxin
title_fullStr Human mitochondrial ferritin improves respiratory function in yeast mutants deficient in iron–sulfur cluster biogenesis, but is not a functional homologue of yeast frataxin
title_full_unstemmed Human mitochondrial ferritin improves respiratory function in yeast mutants deficient in iron–sulfur cluster biogenesis, but is not a functional homologue of yeast frataxin
title_short Human mitochondrial ferritin improves respiratory function in yeast mutants deficient in iron–sulfur cluster biogenesis, but is not a functional homologue of yeast frataxin
title_sort human mitochondrial ferritin improves respiratory function in yeast mutants deficient in iron–sulfur cluster biogenesis, but is not a functional homologue of yeast frataxin
topic Original Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3426411/
https://www.ncbi.nlm.nih.gov/pubmed/22950017
http://dx.doi.org/10.1002/mbo3.18
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