2010
DOI: 10.3324/haematol.2009.020123
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Heme controls ferroportin1 (FPN1) transcription involving Bach1, Nrf2 and a MARE/ARE sequence motif at position -7007 of the FPN1 promoter

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Cited by 245 publications
(228 citation statements)
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“…Ferroportin is expressed at high concentrations on duodenal enterocytes, placenta, hepatocytes, and macrophages (1012) and is an essential component of systemic iron homeostasis (13). Ferroportin is regulated by at least three mechanisms: transcriptional regulation, which controls levels (14) and splice variants (15) of the messenger RNA (mRNA); translational control, which regulates ferroportin through an iron-regulatory element in the 5′ untranslated region of ferroportin mRNA (16); and organismal iron status, which regulates ferroportin-mediated iron efflux through a direct interaction of ferroportin with the peptide hormone hepcidin (17). Hepcidin is secreted by the liver and binds to a specific extracellular loop domain on ferroportin (18).…”
Section: Introductionmentioning
confidence: 99%
“…Ferroportin is expressed at high concentrations on duodenal enterocytes, placenta, hepatocytes, and macrophages (1012) and is an essential component of systemic iron homeostasis (13). Ferroportin is regulated by at least three mechanisms: transcriptional regulation, which controls levels (14) and splice variants (15) of the messenger RNA (mRNA); translational control, which regulates ferroportin through an iron-regulatory element in the 5′ untranslated region of ferroportin mRNA (16); and organismal iron status, which regulates ferroportin-mediated iron efflux through a direct interaction of ferroportin with the peptide hormone hepcidin (17). Hepcidin is secreted by the liver and binds to a specific extracellular loop domain on ferroportin (18).…”
Section: Introductionmentioning
confidence: 99%
“…However, our current understanding of the transcriptional regulation of FPN is still rather limited. Burgeoning studies have documented that HIF-2α, Nrf2 and MTF-1 transcriptionally modulate FPN expression in mouse macrophages and other non-tumor cells [21][22][23]. Other than these, the upstream signaling responsible for FPN's transcriptional regulation remains elusive, especially in tumor cells.…”
Section: Introductionmentioning
confidence: 99%
“…Fpn is most highly expressed in cells that play a major role in iron acquisition: duodenal enterocytes, macrophages, hepatocytes and syncytial trophoblasts. Fpn, however, can be expressed on a wide variety of other cell types in response to heme 3,4 or iron. [5][6][7] Iron can regulate Fpn expression through transcriptional and translational mechanisms.…”
Section: Introductionmentioning
confidence: 99%