Novel insights into iron metabolism by integrating deletome and transcriptome analysis in an iron deficiency model of the yeast <it>Saccharomyces cerevisiae</it>

Novel insights into iron metabolism by integrating deletome and transcriptome analysis in an iron deficiency model of the yeast <it>Saccharomyces cerevisiae</it>

<p>Abstract</p> <p>Background</p> <p>Iron-deficiency anemia is the most prevalent form of anemia world-wide. The yeast <it>Saccharomyces cerevisiae </it>has been used as a model of cellular iron deficiency, in part because many of its cellular pathways are c...

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Main Authors: Arkin Adam P, Loguinov Alex V, Holman Patricia, Jaramillo Daniel, Oh Eric, Kim Jeung Hyoun, Jo William J, Nislow Corey, Giaever Guri, Vulpe Chris D
Format: Article
Language:English
Published: BMC 2009-03-01
Series:BMC Genomics
Online Access:http://www.biomedcentral.com/1471-2164/10/130
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author Arkin Adam P
Loguinov Alex V
Holman Patricia
Jaramillo Daniel
Oh Eric
Kim Jeung Hyoun
Jo William J
Nislow Corey
Giaever Guri
Vulpe Chris D
author_facet Arkin Adam P
Loguinov Alex V
Holman Patricia
Jaramillo Daniel
Oh Eric
Kim Jeung Hyoun
Jo William J
Nislow Corey
Giaever Guri
Vulpe Chris D
author_sort Arkin Adam P
collection DOAJ
description <p>Abstract</p> <p>Background</p> <p>Iron-deficiency anemia is the most prevalent form of anemia world-wide. The yeast <it>Saccharomyces cerevisiae </it>has been used as a model of cellular iron deficiency, in part because many of its cellular pathways are conserved. To better understand how cells respond to changes in iron availability, we profiled the yeast genome with a parallel analysis of homozygous deletion mutants to identify essential components and cellular processes required for optimal growth under iron-limited conditions. To complement this analysis, we compared those genes identified as important for fitness to those that were differentially-expressed in the same conditions. The resulting analysis provides a global perspective on the cellular processes involved in iron metabolism.</p> <p>Results</p> <p>Using functional profiling, we identified several genes known to be involved in high affinity iron uptake, in addition to novel genes that may play a role in iron metabolism. Our results provide support for the primary involvement in iron homeostasis of vacuolar and endosomal compartments, as well as vesicular transport to and from these compartments. We also observed an unexpected importance of the peroxisome for growth in iron-limited media. Although these components were essential for growth in low-iron conditions, most of them were not differentially-expressed. Genes with altered expression in iron deficiency were mainly associated with iron uptake and transport mechanisms, with little overlap with those that were functionally required. To better understand this relationship, we used expression-profiling of selected mutants that exhibited slow growth in iron-deficient conditions, and as a result, obtained additional insight into the roles of <it>CTI6</it>, <it>DAP1</it>, <it>MRS4 </it>and <it>YHR045W </it>in iron metabolism.</p> <p>Conclusion</p> <p>Comparison between functional and gene expression data in iron deficiency highlighted the complementary utility of these two approaches to identify important functional components. This should be taken into consideration when designing and analyzing data from these type of studies. We used this and other published data to develop a molecular interaction network of iron metabolism in yeast.</p>
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spelling doaj.art-3c7ecfc5f1904367926b63b1e3b4e8472022-12-22T03:06:53ZengBMCBMC Genomics1471-21642009-03-0110113010.1186/1471-2164-10-130Novel insights into iron metabolism by integrating deletome and transcriptome analysis in an iron deficiency model of the yeast <it>Saccharomyces cerevisiae</it>Arkin Adam PLoguinov Alex VHolman PatriciaJaramillo DanielOh EricKim Jeung HyounJo William JNislow CoreyGiaever GuriVulpe Chris D<p>Abstract</p> <p>Background</p> <p>Iron-deficiency anemia is the most prevalent form of anemia world-wide. The yeast <it>Saccharomyces cerevisiae </it>has been used as a model of cellular iron deficiency, in part because many of its cellular pathways are conserved. To better understand how cells respond to changes in iron availability, we profiled the yeast genome with a parallel analysis of homozygous deletion mutants to identify essential components and cellular processes required for optimal growth under iron-limited conditions. To complement this analysis, we compared those genes identified as important for fitness to those that were differentially-expressed in the same conditions. The resulting analysis provides a global perspective on the cellular processes involved in iron metabolism.</p> <p>Results</p> <p>Using functional profiling, we identified several genes known to be involved in high affinity iron uptake, in addition to novel genes that may play a role in iron metabolism. Our results provide support for the primary involvement in iron homeostasis of vacuolar and endosomal compartments, as well as vesicular transport to and from these compartments. We also observed an unexpected importance of the peroxisome for growth in iron-limited media. Although these components were essential for growth in low-iron conditions, most of them were not differentially-expressed. Genes with altered expression in iron deficiency were mainly associated with iron uptake and transport mechanisms, with little overlap with those that were functionally required. To better understand this relationship, we used expression-profiling of selected mutants that exhibited slow growth in iron-deficient conditions, and as a result, obtained additional insight into the roles of <it>CTI6</it>, <it>DAP1</it>, <it>MRS4 </it>and <it>YHR045W </it>in iron metabolism.</p> <p>Conclusion</p> <p>Comparison between functional and gene expression data in iron deficiency highlighted the complementary utility of these two approaches to identify important functional components. This should be taken into consideration when designing and analyzing data from these type of studies. We used this and other published data to develop a molecular interaction network of iron metabolism in yeast.</p>http://www.biomedcentral.com/1471-2164/10/130
spellingShingle Arkin Adam P
Loguinov Alex V
Holman Patricia
Jaramillo Daniel
Oh Eric
Kim Jeung Hyoun
Jo William J
Nislow Corey
Giaever Guri
Vulpe Chris D
Novel insights into iron metabolism by integrating deletome and transcriptome analysis in an iron deficiency model of the yeast <it>Saccharomyces cerevisiae</it>
BMC Genomics
title Novel insights into iron metabolism by integrating deletome and transcriptome analysis in an iron deficiency model of the yeast <it>Saccharomyces cerevisiae</it>
title_full Novel insights into iron metabolism by integrating deletome and transcriptome analysis in an iron deficiency model of the yeast <it>Saccharomyces cerevisiae</it>
title_fullStr Novel insights into iron metabolism by integrating deletome and transcriptome analysis in an iron deficiency model of the yeast <it>Saccharomyces cerevisiae</it>
title_full_unstemmed Novel insights into iron metabolism by integrating deletome and transcriptome analysis in an iron deficiency model of the yeast <it>Saccharomyces cerevisiae</it>
title_short Novel insights into iron metabolism by integrating deletome and transcriptome analysis in an iron deficiency model of the yeast <it>Saccharomyces cerevisiae</it>
title_sort novel insights into iron metabolism by integrating deletome and transcriptome analysis in an iron deficiency model of the yeast it saccharomyces cerevisiae it
url http://www.biomedcentral.com/1471-2164/10/130
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