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Iron Availability in Tissue Microenvironment: The Key Role of Ferroportin

Elena Gammella, Margherita Correnti, Gaetano Cairo, Stefania Recalcati

2021International Journal of Molecular Sciences23 citationsDOIOpen Access PDF

Abstract

Body iron levels are regulated by hepcidin, a liver-derived peptide that exerts its function by controlling the presence of ferroportin (FPN), the sole cellular iron exporter, on the cell surface. Hepcidin binding leads to FPN internalization and degradation, thereby inhibiting iron release, in particular from iron-absorbing duodenal cells and macrophages involved in iron recycling. Disruption in this regulatory mechanism results in a variety of disorders associated with iron-deficiency or overload. In recent years, increasing evidence has emerged to indicate that, in addition to its role in systemic iron metabolism, FPN may play an important function in local iron control, such that its dysregulation may lead to tissue damage despite unaltered systemic iron homeostasis. In this review, we focus on recent discoveries to discuss the role of FPN-mediated iron export in the microenvironment under both physiological and pathological conditions.

Topics & Concepts

FerroportinHepcidinInternalizationCell biologyFunction (biology)IntracellularIron deficiencyIron homeostasisHomeostasisMetabolismChemistryCellBiologyBiochemistryInflammationImmunologyAnemiaMedicineInternal medicineIron Metabolism and DisordersHemoglobinopathies and Related DisordersErythropoietin and Anemia Treatment
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