Literature DB >> 20627190

Mechanisms for the shuttling of plasma non-transferrin-bound iron (NTBI) onto deferoxamine by deferiprone.

Patricia Evans1, Reem Kayyali, Robert C Hider, John Eccleston, John B Porter.   

Abstract

In iron overload conditions, plasma contains non-transferrin bound iron species, collectively referred to as plasma NTBI. These include iron citrate species, some of which are protein bound. Because NTBI is taken into tissues susceptible to iron loading, its removal by chelation is desirable but only partial using standard deferoxamine (DFO) therapy. Speciation plots suggest that, at clinically achievable concentrations, deferiprone (DFP) will shuttle iron onto DFO to form feroxamine (FO), but whether NTBI chelation by DFO is enhanced to therapeutically relevant rates by DFP is unknown. As FO is highly stable, kinetic measurements of FO formation by high-performance liquid chromatography or by stopped-flow spectrometry are achievable. In serum from thalassemia major patients supplemented with 10 microM DFO, FO formation paralleled NTBI removal but never exceeded 50% of potentially available NTBI; approximately one third of NTBI was chelated rapidly but only 15% of the remainder at 20 h. Addition of DFP increased the magnitude of the slower component, with increments in FO formation equivalent to complete NTBI removal by 8 h. This shuttling effect was absent in serum from healthy control subjects, indicating no transferrin iron removal. Studies with iron citrate solutions also showed biphasic chelation by DFO, the slow component being accelerated by the addition of DFP, with optimal enhancement at 30 microM. Physiological concentrations of albumin also enhanced DFO chelation from iron citrate, and the co-addition of DFP further accelerated this effect. We conclude that at clinically relevant concentrations, DFP enhances plasma NTBI chelation with DFO by rapidly accessing and shuttling NTBI fractions that are otherwise only slowly available to DFO. Copyright (c) 2010 Mosby, Inc. All rights reserved.

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Year:  2010        PMID: 20627190      PMCID: PMC2927975          DOI: 10.1016/j.trsl.2010.05.002

Source DB:  PubMed          Journal:  Transl Res        ISSN: 1878-1810            Impact factor:   7.012


  34 in total

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Review 2.  Secondary iron overload.

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Review 3.  Nature of nontransferrin-bound iron.

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Journal:  Eur J Clin Invest       Date:  2002-03       Impact factor: 4.686

4.  Exploring the "iron shuttle" hypothesis in chelation therapy: effects of combined deferoxamine and deferiprone treatment in hypertransfused rats with labeled iron stores and in iron-loaded rat heart cells in culture.

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Journal:  J Lab Clin Med       Date:  2001-08

Review 5.  Deferoxamine pharmacokinetics.

Authors:  J B Porter
Journal:  Semin Hematol       Date:  2001-01       Impact factor: 3.851

Review 6.  Chelation therapy in beta-thalassemia: an optimistic update.

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9.  Daily labile plasma iron as an indicator of chelator activity in Thalassaemia major patients.

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  10 in total

1.  Timed non-transferrin bound iron determinations probe the origin of chelatable iron pools during deferiprone regimens and predict chelation response.

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4.  Toward optimizing the use of deferasirox: potential benefits of combined use with deferoxamine.

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5.  Intracellular Iron Binding and Antioxidant Activity of Phytochelators.

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6.  Combined chelation therapy with deferasirox and deferoxamine in thalassemia.

Authors:  Ashutosh Lal; John Porter; Nancy Sweeters; Vivian Ng; Patricia Evans; Lynne Neumayr; Gregory Kurio; Paul Harmatz; Elliott Vichinsky
Journal:  Blood Cells Mol Dis       Date:  2012-11-11       Impact factor: 3.039

Review 7.  Iron chelation therapy in transfusion-dependent thalassemia patients: current strategies and future directions.

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8.  Residual erythropoiesis protects against myocardial hemosiderosis in transfusion-dependent thalassemia by lowering labile plasma iron via transient generation of apotransferrin.

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Journal:  Haematologica       Date:  2017-06-22       Impact factor: 9.941

9.  Eltrombopag: a powerful chelator of cellular or extracellular iron(III) alone or combined with a second chelator.

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10.  Clinical and methodological factors affecting non-transferrin-bound iron values using a novel fluorescent bead assay.

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  10 in total

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