Literature DB >> 1381604

Antibodies for denatured human H-ferritin stain only reticuloendothelial cells within the bone marrow.

G Ruggeri1, P Santambrogio, F Bonfiglio, S Levi, G Bugari, R Verardi, M Cazzola, R Invernizzi, L M Zambelli, A Albertini.   

Abstract

Human H-ferritin homopolymer was denatured in sodium dodecyl sulphate and injected in mice to obtain antibodies for dissociated H-subunit. The antisera and Moabs obtained were specific for the denatured H-chain with no cross-reactivity with assembled ferritins in immunoblotting experiments. In contrast the Moabs for native recombinant H-ferritin are specific for the assembled ferritin molecules with weak cross-reactivity with the denatured H-subunits. The epitope recognized by one of the anti-denatured H-chain Moabs was mapped on the C-terminal helix of ferritin. The antibodies were used to study H-ferritin conformation in cells. In immunocytochemistry experiments the antibodies for denatured H-ferritin stained HeLa and K562 cells weakly, with a different intensity and pattern to those obtained with anti-native H-ferritin antibody. In human bone marrow smears the anti-denatured ferritin antibodies stained only reticuloendothelial cells, and did not recognize the H-ferritin rich immature erythroblasts. It is concluded that assembled and denatured H-ferritins are immunogenically distinct, and that erythroid and reticuloendothelial cells within the bone marrow contain H-ferritin in different conformations.

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Year:  1992        PMID: 1381604     DOI: 10.1111/j.1365-2141.1992.tb08183.x

Source DB:  PubMed          Journal:  Br J Haematol        ISSN: 0007-1048            Impact factor:   6.998


  2 in total

1.  A mutation, in the iron-responsive element of H ferritin mRNA, causing autosomal dominant iron overload.

Authors:  J Kato; K Fujikawa; M Kanda; N Fukuda; K Sasaki; T Takayama; M Kobune; K Takada; R Takimoto; H Hamada; T Ikeda; Y Niitsu
Journal:  Am J Hum Genet       Date:  2001-05-24       Impact factor: 11.025

2.  Denatured H-ferritin subunit is a major constituent of haemosiderin in the liver of patients with iron overload.

Authors:  E Miyazaki; J Kato; M Kobune; K Okumura; K Sasaki; N Shintani; P Arosio; Y Niitsu
Journal:  Gut       Date:  2002-03       Impact factor: 23.059

  2 in total

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