Literature DB >> 1911786

Receptor-modulated iron release from transferrin: differential effects on N- and C-terminal sites.

P K Bali1, P Aisen.   

Abstract

Iron release to PPi from N- and C-terminal monoferric transferrins and their complexes with transferrin receptor has been studied at pH 7.4 and 5.6 in 0.05 M HEPES or MES/0.1 M NaCl/0.01 M CHAPS at 25 degrees C. The two sites exhibit kinetic heterogeneity in releasing iron. The N-terminal form is slightly less labile than its C-terminal counterpart at pH 7.4, but much more facile in releasing iron at pH 5.6. At pH 7.4, iron removal by 0.05 M pyrophosphate from each form of monoferric transferrin complexed to the receptor is considerably slower than from the corresponding free monoferric transferrin. However, at pH 5.6, complexation of transferrin to its receptor affects the two forms differently. The rate of iron release to 0.005 M pyrophosphate by the N-terminal species is substantially the same whether transferrin is free or bound to the receptor. In contrast, the C-terminal form releases iron much faster when complexed to the receptor than when free. Urea/PAGE analysis of iron removal from free and receptor-complexed diferric transferrin at pH 5.6 reveals that its C-terminal site is also more labile in the complex, but its N-terminal site is more labile in free diferric transferrin. Thus, the newly discovered role of transferrin receptor in modulating iron release from transferrin predominantly involves the C-terminal site. This observation helps explain the prevalence of circulating N-terminal monoferric transferrin in the human circulation.

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Year:  1991        PMID: 1911786     DOI: 10.1021/bi00105a019

Source DB:  PubMed          Journal:  Biochemistry        ISSN: 0006-2960            Impact factor:   3.162


  27 in total

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Review 2.  The long history of iron in the Universe and in health and disease.

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3.  Terephthalamide-containing ligands: fast removal of iron from transferrin.

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Review 4.  Dealing with iron: common structural principles in proteins that transport iron and heme.

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5.  Human serum transferrin: a tale of two lobes. Urea gel and steady state fluorescence analysis of recombinant transferrins as a function of pH, time, and the soluble portion of the transferrin receptor.

Authors:  Shaina L Byrne; Anne B Mason
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Review 6.  Hepatic iron overload and hepatocellular carcinoma.

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7.  Interaction of transferrin and its iron-binding fragments with heparin.

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8.  Computational structure models of apo and diferric transferrin-transferrin receptor complexes.

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Journal:  Protein J       Date:  2009-12       Impact factor: 2.371

9.  Inequivalent contribution of the five tryptophan residues in the C-lobe of human serum transferrin to the fluorescence increase when iron is released.

Authors:  Nicholas G James; Shaina L Byrne; Ashley N Steere; Valerie C Smith; Ross T A MacGillivray; Anne B Mason
Journal:  Biochemistry       Date:  2009-04-07       Impact factor: 3.162

10.  Oxidative metal release from metallothionein via zinc-thiol/disulfide interchange.

Authors:  W Maret
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