hmSOD1 gene mutation‐induced disturbance in iron metabolism is mediated by impairment of Akt signalling pathway

hmSOD1 gene mutation‐induced disturbance in iron metabolism is mediated by impairment of Akt signalling pathway

Abstract Background Recently, skeletal muscle atrophy, impairment of iron metabolism, and insulin signalling have been reported in rats suffering from amyotrophic lateral sclerosis (ALS). However, the interrelationship between these changes has not been studied. We hypothesize that an impaired Akt–F...

Full description

Bibliographic Details
Main Authors: Malgorzata Halon‐Golabek, Andzelika Borkowska, Jan J. Kaczor, Wieslaw Ziolkowski, Damian J. Flis, Narcyz Knap, Kajetan Kasperuk, Jedrzej Antosiewicz
Format: Article
Language:English
Published: Wiley 2018-06-01
Series:Journal of Cachexia, Sarcopenia and Muscle
Subjects:
ALS
Oxidative stress
p66Shc
Ferritin
FOXO3a
Muscle iron metabolism
Online Access:https://doi.org/10.1002/jcsm.12283
id doaj-bfa4cc2778d143ea9e8da409b832f588
record_format Article
spelling doaj-bfa4cc2778d143ea9e8da409b832f5882020-11-25T00:26:00ZengWileyJournal of Cachexia, Sarcopenia and Muscle2190-59912190-60092018-06-019355756910.1002/jcsm.12283hmSOD1 gene mutation‐induced disturbance in iron metabolism is mediated by impairment of Akt signalling pathwayMalgorzata Halon‐Golabek0Andzelika Borkowska1Jan J. Kaczor2Wieslaw Ziolkowski3Damian J. Flis4Narcyz Knap5Kajetan Kasperuk6Jedrzej Antosiewicz7Department of Physiotherapy Medical University of Gdansk Gdansk 80‐211 PolandDepartment of Bioenergetics and Physiology of Exercise Medical University of Gdansk Gdansk 80‐211 PolandDepartment of Bioenergetics and Physiology of Exercise Medical University of Gdansk Gdansk 80‐211 PolandDepartment of Bioenergetics and Nutrition Gdansk University of Physical Education and Sport Gdansk 80‐336 PolandDepartment of Bioenergetics and Physiology of Exercise Medical University of Gdansk Gdansk 80‐211 PolandDepartment of Medical Chemistry Medical University of Gdansk Gdansk 80‐211 PolandDepartment of Bioenergetics and Physiology of Exercise Medical University of Gdansk Gdansk 80‐211 PolandDepartment of Bioenergetics and Physiology of Exercise Medical University of Gdansk Gdansk 80‐211 PolandAbstract Background Recently, skeletal muscle atrophy, impairment of iron metabolism, and insulin signalling have been reported in rats suffering from amyotrophic lateral sclerosis (ALS). However, the interrelationship between these changes has not been studied. We hypothesize that an impaired Akt–FOXO3a signalling pathway triggers changes in the iron metabolism in the muscles of transgenic animals. Methods In the present study, we used transgenic rats bearing the G93A hmSOD1 gene and their non‐transgenic littermates. The study was performed on the muscles taken from animals at three different stages of the disease: asymptomatic (ALS I), the onset of the disease (ALS II), and the terminal stage of the disease (ALS III). In order to study the molecular mechanism of changes in iron metabolism, we used SH‐SY5Y and C2C12 cell lines stably transfected with pcDNA3.1, SOD1 WT and SOD1 G93A, or FOXO3a TM‐ER. Results A significant decrease in P‐Akt level and changes in iron metabolism were observed even in the group of ALS I animals. This was accompanied by an increase in the active form of FOXO3a, up‐regulation of atrogin‐1, and catalase. However, significant muscle atrophy was observed in ALS II animals. An increase in ferritin L and H was accompanied by a rise in PCBP1 and APP protein levels. In SH‐SY5Y cells stably expressing SOD1 or SOD1 G93A, we observed elevated levels of ferritin L and H and non‐haem iron. Interestingly, insulin treatment significantly down‐regulated ferritin L and H proteins in the cell. Conversely, cells transfected with small interfering RNA against Akt 1, 2, 3, respectively, showed a significant increase in the ferritin and FOXO3a levels. In order to assess the role of FOXO3a in the ferritin expression, we constructed a line of SH‐SY5Y cells that expressed a fusion protein made of FOXO3a fused at the C‐terminus with the ligand‐binding domain of the oestrogen receptor (TM‐ER) being activated by 4‐hydroxytamoxifen. Treatment of the cells with 4‐hydroxytamoxifen significantly up‐regulated ferritin L and H proteins level. Conclusions Our data suggest that impairment of insulin signalling and iron metabolism in the skeletal muscle precedes muscle atrophy and is mediated by changes in Akt/FOXO3a signalling pathways.https://doi.org/10.1002/jcsm.12283ALSOxidative stressp66ShcFerritinFOXO3aMuscle iron metabolism
collection DOAJ
language English
format Article
sources DOAJ
author Malgorzata Halon‐Golabek
Andzelika Borkowska
Jan J. Kaczor
Wieslaw Ziolkowski
Damian J. Flis
Narcyz Knap
Kajetan Kasperuk
Jedrzej Antosiewicz
spellingShingle Malgorzata Halon‐Golabek
Andzelika Borkowska
Jan J. Kaczor
Wieslaw Ziolkowski
Damian J. Flis
Narcyz Knap
Kajetan Kasperuk
Jedrzej Antosiewicz
hmSOD1 gene mutation‐induced disturbance in iron metabolism is mediated by impairment of Akt signalling pathway
Journal of Cachexia, Sarcopenia and Muscle
ALS
Oxidative stress
p66Shc
Ferritin
FOXO3a
Muscle iron metabolism
author_facet Malgorzata Halon‐Golabek
Andzelika Borkowska
Jan J. Kaczor
Wieslaw Ziolkowski
Damian J. Flis
Narcyz Knap
Kajetan Kasperuk
Jedrzej Antosiewicz
author_sort Malgorzata Halon‐Golabek
title hmSOD1 gene mutation‐induced disturbance in iron metabolism is mediated by impairment of Akt signalling pathway
title_short hmSOD1 gene mutation‐induced disturbance in iron metabolism is mediated by impairment of Akt signalling pathway
title_full hmSOD1 gene mutation‐induced disturbance in iron metabolism is mediated by impairment of Akt signalling pathway
title_fullStr hmSOD1 gene mutation‐induced disturbance in iron metabolism is mediated by impairment of Akt signalling pathway
title_full_unstemmed hmSOD1 gene mutation‐induced disturbance in iron metabolism is mediated by impairment of Akt signalling pathway
title_sort hmsod1 gene mutation‐induced disturbance in iron metabolism is mediated by impairment of akt signalling pathway
publisher Wiley
series Journal of Cachexia, Sarcopenia and Muscle
issn 2190-5991
2190-6009
publishDate 2018-06-01
description Abstract Background Recently, skeletal muscle atrophy, impairment of iron metabolism, and insulin signalling have been reported in rats suffering from amyotrophic lateral sclerosis (ALS). However, the interrelationship between these changes has not been studied. We hypothesize that an impaired Akt–FOXO3a signalling pathway triggers changes in the iron metabolism in the muscles of transgenic animals. Methods In the present study, we used transgenic rats bearing the G93A hmSOD1 gene and their non‐transgenic littermates. The study was performed on the muscles taken from animals at three different stages of the disease: asymptomatic (ALS I), the onset of the disease (ALS II), and the terminal stage of the disease (ALS III). In order to study the molecular mechanism of changes in iron metabolism, we used SH‐SY5Y and C2C12 cell lines stably transfected with pcDNA3.1, SOD1 WT and SOD1 G93A, or FOXO3a TM‐ER. Results A significant decrease in P‐Akt level and changes in iron metabolism were observed even in the group of ALS I animals. This was accompanied by an increase in the active form of FOXO3a, up‐regulation of atrogin‐1, and catalase. However, significant muscle atrophy was observed in ALS II animals. An increase in ferritin L and H was accompanied by a rise in PCBP1 and APP protein levels. In SH‐SY5Y cells stably expressing SOD1 or SOD1 G93A, we observed elevated levels of ferritin L and H and non‐haem iron. Interestingly, insulin treatment significantly down‐regulated ferritin L and H proteins in the cell. Conversely, cells transfected with small interfering RNA against Akt 1, 2, 3, respectively, showed a significant increase in the ferritin and FOXO3a levels. In order to assess the role of FOXO3a in the ferritin expression, we constructed a line of SH‐SY5Y cells that expressed a fusion protein made of FOXO3a fused at the C‐terminus with the ligand‐binding domain of the oestrogen receptor (TM‐ER) being activated by 4‐hydroxytamoxifen. Treatment of the cells with 4‐hydroxytamoxifen significantly up‐regulated ferritin L and H proteins level. Conclusions Our data suggest that impairment of insulin signalling and iron metabolism in the skeletal muscle precedes muscle atrophy and is mediated by changes in Akt/FOXO3a signalling pathways.
topic ALS
Oxidative stress
p66Shc
Ferritin
FOXO3a
Muscle iron metabolism
url https://doi.org/10.1002/jcsm.12283
work_keys_str_mv AT malgorzatahalongolabek hmsod1genemutationinduceddisturbanceinironmetabolismismediatedbyimpairmentofaktsignallingpathway
AT andzelikaborkowska hmsod1genemutationinduceddisturbanceinironmetabolismismediatedbyimpairmentofaktsignallingpathway
AT janjkaczor hmsod1genemutationinduceddisturbanceinironmetabolismismediatedbyimpairmentofaktsignallingpathway
AT wieslawziolkowski hmsod1genemutationinduceddisturbanceinironmetabolismismediatedbyimpairmentofaktsignallingpathway
AT damianjflis hmsod1genemutationinduceddisturbanceinironmetabolismismediatedbyimpairmentofaktsignallingpathway
AT narcyzknap hmsod1genemutationinduceddisturbanceinironmetabolismismediatedbyimpairmentofaktsignallingpathway
AT kajetankasperuk hmsod1genemutationinduceddisturbanceinironmetabolismismediatedbyimpairmentofaktsignallingpathway
AT jedrzejantosiewicz hmsod1genemutationinduceddisturbanceinironmetabolismismediatedbyimpairmentofaktsignallingpathway
_version_ 1725346435048669184

Similar Items