Literature DB >> 6694350

Studies of iron overload. Rat liver siderosome ferritin.

G W Richter.   

Abstract

To investigate storage of ferritin and its transition to hemosiderin under conditions of iron overload, rats were either given multiple injections of iron dextran over 4 to 5 weeks or fed a diet containing 1.3% Fe as ferric ammonium citrate for 60 days. Then, preparations of liver siderosomes (heavily iron-laden lysosomes) were examined for content of buffer-soluble ferritin and buffer-insoluble, ferritin-related protein, total nonheme iron and protein, cathepsin D activity, and ability to incorporate 14C-leucine into ferritin. Total liver nonheme iron, ferritin protein and iron, and cathepsin D activity were also determined. Although parenteral iron loading produced higher total nonheme iron in livers than dietary loading, the iron content of ferritin was approximately 20% in both groups, reflecting saturation of ferritin with iron. Siderosome nonheme iron content was greater than 40% in relation to protein. The siderosomes contained little buffer-soluble ferritin; on isoelectric focusing this was composed of isoferritins present also in cytosol ferritin. Buffer-insoluble ferritin protein, identified in siderosomes by immunofluorescence, was solubilized and found to contain immunoreactive material corresponding to L and H subunits of buffer-soluble ferritin. Transmission electron microscopy indicated the presence of relatively large quantities of "ferritin" in siderosomes, and it is argued that this was mostly buffer insoluble (denatured) or represented ferritin [FeOOH]x cores divested of protein shells. Although siderosomes had substantial cathepsin D activity, the known resistance of ferritin to this and other proteases makes it unlikely that proteolysis is an early event in the decomposition of ferritin in siderosomes. Heavily iron-laden siderosomes did not take up newly labeled ferritin or ferritin protein or 14C-precursor within 24 hours of labeling, when 14C-labeled ferritin was abundant in cytosol. The author proposes a sequence of steps leading from sequestration of buffer-soluble cytosol ferritin to storage of insoluble "hemosiderin."

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Year:  1984        PMID: 6694350

Source DB:  PubMed          Journal:  Lab Invest        ISSN: 0023-6837            Impact factor:   5.662


  13 in total

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4.  Aceruloplasminemia: retinal histopathologic manifestations and iron-mediated melanosome degradation.

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5.  Quantitative analysis of immunogold labelling for ferritin in liver from control and iron-overloaded rats.

Authors:  P J Cooper; T C Iancu; R J Ward; K M Guttridge; T J Peters
Journal:  Histochem J       Date:  1988-09

6.  Mimicking liver iron overload using liposomal ferritin preparations.

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7.  A new form of ferritin heterogeneity explained. Isolation and identification of a nineteen-amino-acid-residue fragment from siderosomal ferritin of rat liver.

Authors:  S C Andrews; A Treffry; P M Harrison
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8.  Siderosomal ferritin. The missing link between ferritin and haemosiderin?

Authors:  S C Andrews; A Treffry; P M Harrison
Journal:  Biochem J       Date:  1987-07-15       Impact factor: 3.857

9.  Studies on haemosiderin and ferritin from iron-loaded rat liver.

Authors:  S C Andrews; M C Brady; A Treffry; J M Williams; S Mann; M I Cleton; W de Bruijn; P M Harrison
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10.  Effect of phlebotomy on the ferritin iron content in the rat liver as determined morphometrically with the use of electron energy loss spectroscopy.

Authors:  M I Cleton; L J Mostert; L W Sorber; A A de Jong; C M de Jeu-Jaspars; W C de Bruijn
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