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Nature of non-transferrin-bound iron: studies on iron citrate complexes and thalassemic sera
Authors:Robert W. Evans  Roozina Rafique  Adel Zarea  Chiara Rapisarda  Richard Cammack  Patricia J. Evans  John B. Porter  Robert C. Hider
Affiliation:(1) Metalloprotein Research Group, Nutritional Sciences Division, King’s College London, New Hunt’s House, London, SE1 1UL, UK;(2) Department of Haematology, University College London, 98 Chenies Mews, London, WC1E 2HC, UK;(3) Drug Discovery Group, Pharmaceutical Sciences Research Division, King’s College London, Stamford Street, London, SE1 9NN, UK;(4) Molecular Biophysics Group, Pharmaceutical Sciences Research Division, King’s College London, Stamford Street, London, SE1 9NN, UK
Abstract:Despite its importance in iron-overload diseases, little is known about the composition of plasma non-transferrin-bound iron (NTBI). Using 30-kDa ultrafiltration, plasma from thalassemic patients consisted of both filterable and non-filterable NTBI, the filterable fraction representing less than 10% NTBI. Low filterability could result from protein binding or NTBI species exceeding 30 kDa. The properties of iron citrate and its interaction with albumin were therefore investigated, as these represent likely NTBI species. Iron permeated 5- or 12-kDa ultrafiltration units completely when complexes were freshly prepared and citrate exceeded iron by tenfold, whereas with 30-kDa ultrafiltration units, permeation approached 100% at all molar ratios. A g = 4.3 electron paramagnetic resonance signal, characteristic of mononuclear iron, was detectable only with iron-to-citrate ratios above 1:100. The ability of both desferrioxamine and 1,2-dimethyl-3-hydroxypyridin-4-one to chelate iron in iron citrate complexes also increased with increasing ratios of citrate to iron. Incremental molar excesses of citrate thus favour the progressive appearance of chelatable lower molecular weight iron oligomers, dimers and ultimately monomers. Filtration of iron citrate in the presence of albumin showed substantial binding to albumin across a wide range of iron-to-citrate ratios and also increased accessibility of iron to chelators, reflecting a shift towards smaller oligomeric species. However, in vitro experiments using immunodepletion or absorption of albumin to Cibacron blue–Sepharose indicate that iron is only loosely bound in iron citrate–albumin complexes and that NTBI is unlikely to be albumin-bound to any significant extent in thalassemic sera.
Keywords:Albumin  Iron chelators  Iron citrate  Non-transferrin-bound iron  Thalassemia
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