A novel neuroferritinopathy mouse model (FTL 498InsTC) shows progressive brain iron dysregulation, morphological signs of early neurodegeneration and motor coordination deficits

Neuroferritinopathy is a rare genetic disease with a dominant autosomal transmission caused by mutations of the ferritin light chain gene (FTL). It belongs to Neurodegeneration with Brain Iron Accumulation, a group of disorders where iron dysregulation is tightly associated with neurodegeneration. W...

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Autores principales: Maccarinelli, Federica, Pagani, Antonella, Cozzi, Anna, Codazzi, Franca, Di Giacomo, Giuseppina, Capoccia, Sara, Rapino, Stefania, Finazzi, Dario, Politi, Letterio Salvatore, Cirulli, Francesca, Giorgio, Marco, Cremona, Ottavio, Grohovaz, Fabio, Levi, Sonia
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Academic Press 2015
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4642750/
https://www.ncbi.nlm.nih.gov/pubmed/25447222
http://dx.doi.org/10.1016/j.nbd.2014.10.023
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author Maccarinelli, Federica
Pagani, Antonella
Cozzi, Anna
Codazzi, Franca
Di Giacomo, Giuseppina
Capoccia, Sara
Rapino, Stefania
Finazzi, Dario
Politi, Letterio Salvatore
Cirulli, Francesca
Giorgio, Marco
Cremona, Ottavio
Grohovaz, Fabio
Levi, Sonia
author_facet Maccarinelli, Federica
Pagani, Antonella
Cozzi, Anna
Codazzi, Franca
Di Giacomo, Giuseppina
Capoccia, Sara
Rapino, Stefania
Finazzi, Dario
Politi, Letterio Salvatore
Cirulli, Francesca
Giorgio, Marco
Cremona, Ottavio
Grohovaz, Fabio
Levi, Sonia
author_sort Maccarinelli, Federica
collection PubMed
description Neuroferritinopathy is a rare genetic disease with a dominant autosomal transmission caused by mutations of the ferritin light chain gene (FTL). It belongs to Neurodegeneration with Brain Iron Accumulation, a group of disorders where iron dysregulation is tightly associated with neurodegeneration. We studied the 498–499InsTC mutation which causes the substitution of the last 9 amino acids and an elongation of extra 16 amino acids at the C-terminus of L-ferritin peptide. An analysis with cyclic voltammetry on the purified protein showed that this structural modification severely reduces the ability of the protein to store iron. In order to analyze the impact of the mutation in vivo, we generated mouse models for the some pathogenic human FTL gene in FVB and C57BL/6J strains. Transgenic mice in the FVB background showed high accumulation of the mutated ferritin in brain where it correlated with increased iron deposition with age, as scored by magnetic resonance imaging. Notably, the accumulation of iron–ferritin bodies was accompanied by signs of oxidative damage. In the C57BL/6 background, both the expression of the mutant ferritin and the iron levels were lower than in the FVB strain. Nevertheless, also these mice showed oxidative alterations in the brain. Furthermore, post-natal hippocampal neurons obtained from these mice experienced a marked increased cell death in response to chronic iron overload and/or acute oxidative stress, in comparison to wild-type neurons. Ultrastructural analyses revealed an accumulation of lipofuscin granules associated with iron deposits, particularly enriched in the cerebellum and striatum of our transgenic mice. Finally, experimental subjects were tested throughout development and aging at 2-, 8- and 18-months for behavioral phenotype. Rotarod test revealed a progressive impaired motor coordination building up with age, FTL mutant old mice showing a shorter latency to fall from the apparatus, according to higher accumulation of iron aggregates in the striatum. Our data show that our 498–499InsTC mouse models recapitulate early pathological and clinical traits of the human neuroferritinopathy, thus providing a valuable model for the study of the disease. Finally, we propose a mechanistic model of lipofuscine formation that can account for the etiopathogenesis of human neuroferritinopathy.
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spelling pubmed-46427502015-12-03 A novel neuroferritinopathy mouse model (FTL 498InsTC) shows progressive brain iron dysregulation, morphological signs of early neurodegeneration and motor coordination deficits Maccarinelli, Federica Pagani, Antonella Cozzi, Anna Codazzi, Franca Di Giacomo, Giuseppina Capoccia, Sara Rapino, Stefania Finazzi, Dario Politi, Letterio Salvatore Cirulli, Francesca Giorgio, Marco Cremona, Ottavio Grohovaz, Fabio Levi, Sonia Neurobiol Dis Article Neuroferritinopathy is a rare genetic disease with a dominant autosomal transmission caused by mutations of the ferritin light chain gene (FTL). It belongs to Neurodegeneration with Brain Iron Accumulation, a group of disorders where iron dysregulation is tightly associated with neurodegeneration. We studied the 498–499InsTC mutation which causes the substitution of the last 9 amino acids and an elongation of extra 16 amino acids at the C-terminus of L-ferritin peptide. An analysis with cyclic voltammetry on the purified protein showed that this structural modification severely reduces the ability of the protein to store iron. In order to analyze the impact of the mutation in vivo, we generated mouse models for the some pathogenic human FTL gene in FVB and C57BL/6J strains. Transgenic mice in the FVB background showed high accumulation of the mutated ferritin in brain where it correlated with increased iron deposition with age, as scored by magnetic resonance imaging. Notably, the accumulation of iron–ferritin bodies was accompanied by signs of oxidative damage. In the C57BL/6 background, both the expression of the mutant ferritin and the iron levels were lower than in the FVB strain. Nevertheless, also these mice showed oxidative alterations in the brain. Furthermore, post-natal hippocampal neurons obtained from these mice experienced a marked increased cell death in response to chronic iron overload and/or acute oxidative stress, in comparison to wild-type neurons. Ultrastructural analyses revealed an accumulation of lipofuscin granules associated with iron deposits, particularly enriched in the cerebellum and striatum of our transgenic mice. Finally, experimental subjects were tested throughout development and aging at 2-, 8- and 18-months for behavioral phenotype. Rotarod test revealed a progressive impaired motor coordination building up with age, FTL mutant old mice showing a shorter latency to fall from the apparatus, according to higher accumulation of iron aggregates in the striatum. Our data show that our 498–499InsTC mouse models recapitulate early pathological and clinical traits of the human neuroferritinopathy, thus providing a valuable model for the study of the disease. Finally, we propose a mechanistic model of lipofuscine formation that can account for the etiopathogenesis of human neuroferritinopathy. Academic Press 2015-09 /pmc/articles/PMC4642750/ /pubmed/25447222 http://dx.doi.org/10.1016/j.nbd.2014.10.023 Text en © 2014 The Authors. Published by Elsevier Inc. http://creativecommons.org/licenses/by-nc-nd/3.0/ This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/3.0/).
spellingShingle Article
Maccarinelli, Federica
Pagani, Antonella
Cozzi, Anna
Codazzi, Franca
Di Giacomo, Giuseppina
Capoccia, Sara
Rapino, Stefania
Finazzi, Dario
Politi, Letterio Salvatore
Cirulli, Francesca
Giorgio, Marco
Cremona, Ottavio
Grohovaz, Fabio
Levi, Sonia
A novel neuroferritinopathy mouse model (FTL 498InsTC) shows progressive brain iron dysregulation, morphological signs of early neurodegeneration and motor coordination deficits
title A novel neuroferritinopathy mouse model (FTL 498InsTC) shows progressive brain iron dysregulation, morphological signs of early neurodegeneration and motor coordination deficits
title_full A novel neuroferritinopathy mouse model (FTL 498InsTC) shows progressive brain iron dysregulation, morphological signs of early neurodegeneration and motor coordination deficits
title_fullStr A novel neuroferritinopathy mouse model (FTL 498InsTC) shows progressive brain iron dysregulation, morphological signs of early neurodegeneration and motor coordination deficits
title_full_unstemmed A novel neuroferritinopathy mouse model (FTL 498InsTC) shows progressive brain iron dysregulation, morphological signs of early neurodegeneration and motor coordination deficits
title_short A novel neuroferritinopathy mouse model (FTL 498InsTC) shows progressive brain iron dysregulation, morphological signs of early neurodegeneration and motor coordination deficits
title_sort novel neuroferritinopathy mouse model (ftl 498instc) shows progressive brain iron dysregulation, morphological signs of early neurodegeneration and motor coordination deficits
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4642750/
https://www.ncbi.nlm.nih.gov/pubmed/25447222
http://dx.doi.org/10.1016/j.nbd.2014.10.023
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