Erythroid differentiation and protoporphyrin IX down-regulate frataxin expression in Friend cells: characterization of frataxin expression compared to molecules involved in iron metabolism and hemoglobinization

Abstract: Friedreich ataxia (FA) is caused by decreased frataxin expression that results in mitochondrial iron (Fe) overload. However, the role of frataxin in mammalian Fe metabolism remains unclear. In this investigation we examined the function of frataxin in Fe metabolism by implementing a well-characterized model of erythroid differentiation, namely, Friend cells induced using dimethyl sulfoxide (DMSO). We have characterized the changes in frataxin expression compared to molecules that play key roles in Fe metabolis… Show more

“…Supporting our findings, a direct interaction between purified frataxin and Fech has been reported, suggesting a role for frataxin in heme synthesis (9,20). Indeed, we have suggested that frataxin acts as a metabolic switch to regulate mitochondrial iron utilization between heme and ISC biosynthesis (8). Moreover, an investigation in frataxin knockout mice showed decreased Isu1, Cpox, and Fech mRNA transcripts (not protein levels) (21), which is validated by our findings.…”

“…The precise function of frataxin remains unclear, but it has been implicated in mitochondrial iron metabolism, particularly iron-sulfur cluster (ISC) synthesis (3)(4)(5). Frataxin depletion results in mitochondrial DNA damage, mitochondrial iron accumulation, ISC deficiency, perturbed heme synthesis, and oxidative damage (6)(7)(8)(9). In addition, recent studies have suggested cytosolic iron deficiency in Friedreich's ataxia models, as indicated by increased RNA-binding activity of iron regulatory protein 2, increased expression of transferrin receptor 1 (Tfr1), and decreased cytosolic ferritin (10,11).…”

Elucidation of the mechanism of mitochondrial iron loading in Friedreich's ataxia by analysis of a mouse mutant

“…Supporting our findings, a direct interaction between purified frataxin and Fech has been reported, suggesting a role for frataxin in heme synthesis (9,20). Indeed, we have suggested that frataxin acts as a metabolic switch to regulate mitochondrial iron utilization between heme and ISC biosynthesis (8). Moreover, an investigation in frataxin knockout mice showed decreased Isu1, Cpox, and Fech mRNA transcripts (not protein levels) (21), which is validated by our findings.…”

“…The precise function of frataxin remains unclear, but it has been implicated in mitochondrial iron metabolism, particularly iron-sulfur cluster (ISC) synthesis (3)(4)(5). Frataxin depletion results in mitochondrial DNA damage, mitochondrial iron accumulation, ISC deficiency, perturbed heme synthesis, and oxidative damage (6)(7)(8)(9). In addition, recent studies have suggested cytosolic iron deficiency in Friedreich's ataxia models, as indicated by increased RNA-binding activity of iron regulatory protein 2, increased expression of transferrin receptor 1 (Tfr1), and decreased cytosolic ferritin (10,11).…”

Elucidation of the mechanism of mitochondrial iron loading in Friedreich's ataxia by analysis of a mouse mutant

“…In this latter disease, mutations in the gene encoding frataxin, a protein associated with the mitochondrial inner membrane and involved in (Fe-S) cluster formation, induces Fe accumulation in the mitochondria of non-erythroid cells such as neurons and cardiomyocytes (Campuzano et al, 1996;Pandolfo, 2003). However, no anemia is observed in Friedreich ataxia and Fe does not accumulate in mitochondria of erythroid cells because frataxin levels are low in these cells to favor Fe utilization for heme production (Becker et al, 2002;Napier et al, 2005).…”

Mitochondria in hematopoiesis and hematological diseases

“…This organelle is also responsible for heme and [Fe-S] cluster biosynthesis, and hence, any mitochondrial damage has a large impact on the function of a cell (Cooper and Schapira, 2003). Although the exact function of frataxin has not been determined, it is thought to take part in mitochondrial iron metabolism and [Fe-S] cluster synthesis (Puccio et al, 2001;Becker et al, 2002;Muhlenhoff et al, 2002; for reviews, see Pandolfo, 2002;Alper and Narayanan, 2003;Napier et al, 2005). This correlates with iron accumulation seen in the liver, heart, and spleen of FA patients in a pattern consistent with mitochondria (Sachez-Casis et al, 1976;Lamarche et al, 1993), whereas a decrease in respiratory chain activities of the [Fe-S] cluster-containing complexes I, II, and III is also observed (Rotig et al, 1997;Puccio et al, 2001; for reviews, see Becker and Richardson, 2001;Lodi et al, 2002;Cooper and Schapira, 2003).…”

The Evolution of Iron Chelators for the Treatment of Iron Overload Disease and Cancer