Abstract

Iron is an essential element but is toxic in excess. The concentration of free iron within cells is determined by regulated transmembrane iron import and storage. Malregulation of iron transport results in tissue injury, either from iron deprivation or overload. We propose to identify and characterize genes and proteins that affect the storage of iron in the yeast vacuole and in mammalian lysosomes and determine the mechanisms of high iron toxicity. We will continue our approach of using yeast genetics to identify genes involved in iron metabolism. We have shown that high iron induces a response that up-regulates the expression of the vacuole iron importer Ccc1, which protects yeast cells from iron toxicity. This transcriptional response is regulated by the iron sensitive transcription factor Yap5. We have discovered that transcription of CCC1 is increased by low glucose and iron in a Yap5-independent manner. We will identify the molecules responsible for the Yap5-independent induction of CCC1 and how low glucose affects iron storage. Yeast and mammals also export iron from the vacuole and lysosomes during iron limitation. We will determine if the yeast vacuolar iron exporters, Fet5/Fth1 and Smf3, are regulated post-translationally. Using stringent genetic selection systems, we will identify structural features on transporters that define metal specificity. Vertebrates store iron in ferritin and stored iron can be released from ferritin. Ferrtin can be degraded in the cytosol or in lysosomes, which are the equivalent of yeast vacuoles. We will determine how iron is exported from lysosomes. Iron is stored in ferritin as Fe3+ and must be reduced to Fe2+ to be exported by transporters. We will identify the mechanism of iron reduction and if there is a pool of lysosomal Fe2+. We will determine the role of putative lysosomal iron exporters and if those exporters are regulated at the level of localization, protein stability or activity. Our studies in yeast suggest that iron toxicity can occur both in the presene and absence of oxygen. We will determine the mechanism of oxygen independent iron toxicity. We identified two unique metabolites whose levels increase under conditions of iron toxicity. Through the use of metabolic profiling, we identified two unique metabolites that are only generated by toxic concentrations of iron. We will test the hypothesis that these metabolites are generated by an enzyme that is either mismetallated or altered by high iron. We will also determine if iron-dependent alteration of mitochondrial DNA is a prerequisite for oxygen-dependent iron toxicity. We have shown that alteration of citrate levels exacerbates iron toxicity in yeast. We will determine if alteration of citrate levels affects mammalian iron toxicity.

Public Health Relevance

Iron metabolism is essential for life. Malregulation of iron metabolism leads to disease. This project addresses several issues of central importance to understanding iron homeostasis and how organisms respond to iron limitation or excess. We will determine the mechanisms that regulate iron acquisition and storage. We will also define the mechanisms by which excessive iron accumulation leads to toxicity. Our studies will provide information that may be used to manage and diagnose human diseases due to altered iron metabolism.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Project (R01)
Project #
5R01DK030534-36
Application #
9414027
Study Section
Molecular and Cellular Hematology Study Section (MCH)
Program Officer
Roy, Cindy
Project Start
1982-01-01
Project End
2020-01-31
Budget Start
2018-02-01
Budget End
2020-01-31
Support Year
36
Fiscal Year
2018
Total Cost
Indirect Cost

  Institution

Name
University of Utah
Department
Pathology
Type
Schools of Medicine
DUNS #
009095365
City
Salt Lake City
State
UT
Country
United States
Zip Code
84112

  Publications

Yien, Yvette Y; Shi, Jiahai; Chen, Caiyong et al. (2018) FAM210B is an erythropoietin target and regulates erythroid heme synthesis by controlling mitochondrial iron import and ferrochelatase activity. J Biol Chem 293:19797-19811
Ward, Diane M; Chen, Opal S; Li, Liangtao et al. (2018) Altered sterol metabolism in budding yeast affects mitochondrial iron-sulfur (Fe-S) cluster synthesis. J Biol Chem 293:10782-10795
Meznarich, Jessica A; Draper, Lauren; Christensen, Robert D et al. (2018) Fetal presentation of congenital dyserythropoietic anemia type 1 with novel compound heterozygous CDAN1 mutations. Blood Cells Mol Dis 71:63-66
Li, Liangtao; Ward, Diane M (2018) Iron toxicity in yeast: transcriptional regulation of the vacuolar iron importer Ccc1. Curr Genet 64:413-416
Seguin, Alexandra; Takahashi-Makise, Naoko; Yien, Yvette Y et al. (2017) Reductions in the mitochondrial ABC transporter Abcb10 affect the transcriptional profile of heme biosynthesis genes. J Biol Chem 292:16284-16299
MacQueen, B C; Christensen, R D; Ward, D M et al. (2017) The iron status at birth of neonates with risk factors for developing iron deficiency: a pilot study. J Perinatol 37:436-440
Yaish, Hassan M; Farrell, Colin P; Christensen, Robert D et al. (2017) Two novel mutations in TMPRSS6 associated with iron-refractory iron deficiency anemia in a mother and child. Blood Cells Mol Dis 65:38-40
Li, Liangtao; Kaplan, Jerry; Ward, Diane M (2017) The glucose sensor Snf1 and the transcription factors Msn2 and Msn4 regulate transcription of the vacuolar iron importer gene CCC1 and iron resistance in yeast. J Biol Chem 292:15577-15586
Li, Liangtao; Miao, Ren; Jia, Xuan et al. (2014) Expression of the yeast cation diffusion facilitators Mmt1 and Mmt2 affects mitochondrial and cellular iron homeostasis: evidence for mitochondrial iron export. J Biol Chem 289:17132-41
Ben-Othman, Rym; Flannery, Andrew R; Miguel, Danilo C et al. (2014) Leishmania-mediated inhibition of iron export promotes parasite replication in macrophages. PLoS Pathog 10:e1003901

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