Distinct mechanisms of axonal globule formation in mice expressing human wild type α-synuclein or dementia with Lewy bodies-linked P123H ß-synuclein

Distinct mechanisms of axonal globule formation in mice expressing human wild type α-synuclein or dementia with Lewy bodies-linked P123H ß-synuclein

<p>Abstract</p> <p>Background</p> <p>Axonopathy is critical in the early pathogenesis of neurodegenerative diseases, including Parkinson’s disease (PD) and dementia with Lewy bodies (DLB). Axonal swellings such as globules and spheroids are a distinct feature of axonopa...

Full description

Bibliographic Details
Main Authors: Sekigawa Akio, Fujita Masayo, Sekiyama Kazunari, Takamatsu Yoshiki, Hatano Taku, Rockenstein Edward, La Spada Albert R, Masliah Eliezer, Hashimoto Makoto
Format: Article
Language:English
Published: BMC 2012-09-01
Series:Molecular Brain
Subjects:
α-synuclein
P123H β-synuclein
Parkinson’s disease
Mitochondria
Lysosome
Transgenic mouse
Online Access:http://www.molecularbrain.com/content/5/1/34
id doaj-800de3e6221949089fce428d3349fc6d
record_format Article
spelling doaj-800de3e6221949089fce428d3349fc6d2020-11-25T00:45:01ZengBMCMolecular Brain1756-66062012-09-01513410.1186/1756-6606-5-34Distinct mechanisms of axonal globule formation in mice expressing human wild type α-synuclein or dementia with Lewy bodies-linked P123H ß-synucleinSekigawa AkioFujita MasayoSekiyama KazunariTakamatsu YoshikiHatano TakuRockenstein EdwardLa Spada Albert RMasliah EliezerHashimoto Makoto<p>Abstract</p> <p>Background</p> <p>Axonopathy is critical in the early pathogenesis of neurodegenerative diseases, including Parkinson’s disease (PD) and dementia with Lewy bodies (DLB). Axonal swellings such as globules and spheroids are a distinct feature of axonopathy and our recent study showed that transgenic (tg) mice expressing DLB-linked P123H β-synuclein (P123H βS) were characterized by P123H βS-immunoreactive axonal swellings (P123H βS-globules). Therefore, the objectives of this study were to evaluate α-synuclein (αS)-immunoreactive axonal swellings (αS-globules) in the brains of tg mice expressing human wild-type αS and to compare them with the globules in P123H βS tg mice.</p> <p>Results</p> <p>In αS tg mice, αS-globules were formed in an age-dependent manner in various brain regions, including the thalamus and basal ganglia. These globules were composed of autophagosome-like membranous structures and were reminiscent of P123H βS-globules in P123H βS tg mice. In the αS-globules, frequent clustering and deformation of mitochondria were observed. These changes were associated with oxidative stress, based on staining of nitrated αS and 4-hydroxy-2-nonenal (4-HNE). In accord with the absence of mitochondria in the P123H βS-globules, staining of nitrated αS and 4-HNE in these globules was weaker than that for αS-globules. Leucine-rich repeat kinase 2 (LRRK2), the PARK8 of familial PD, was detected exclusively in αS-globules, suggesting a specific role of this molecule in these globules.</p> <p>Conclusions</p> <p>Lysosomal pathology was similarly observed for both αS- and P123H βS-globules, while oxidative stress was associated with the αS-globules, and to a lesser extent with the P123H βS-globules. Other pathologies, such as mitochondrial alteration and LRRK2 accumulation, were exclusively detected for αS-globules. Collectively, both αS- and P123H βS-globules were formed through similar but distinct pathogenic mechanisms. Our findings suggest that synuclein family members might contribute to diverse axonal pathologies.</p> http://www.molecularbrain.com/content/5/1/34α-synucleinP123H β-synucleinParkinson’s diseaseMitochondriaLysosomeTransgenic mouse
collection DOAJ
language English
format Article
sources DOAJ
author Sekigawa Akio
Fujita Masayo
Sekiyama Kazunari
Takamatsu Yoshiki
Hatano Taku
Rockenstein Edward
La Spada Albert R
Masliah Eliezer
Hashimoto Makoto
spellingShingle Sekigawa Akio
Fujita Masayo
Sekiyama Kazunari
Takamatsu Yoshiki
Hatano Taku
Rockenstein Edward
La Spada Albert R
Masliah Eliezer
Hashimoto Makoto
Distinct mechanisms of axonal globule formation in mice expressing human wild type α-synuclein or dementia with Lewy bodies-linked P123H ß-synuclein
Molecular Brain
α-synuclein
P123H β-synuclein
Parkinson’s disease
Mitochondria
Lysosome
Transgenic mouse
author_facet Sekigawa Akio
Fujita Masayo
Sekiyama Kazunari
Takamatsu Yoshiki
Hatano Taku
Rockenstein Edward
La Spada Albert R
Masliah Eliezer
Hashimoto Makoto
author_sort Sekigawa Akio
title Distinct mechanisms of axonal globule formation in mice expressing human wild type α-synuclein or dementia with Lewy bodies-linked P123H ß-synuclein
title_short Distinct mechanisms of axonal globule formation in mice expressing human wild type α-synuclein or dementia with Lewy bodies-linked P123H ß-synuclein
title_full Distinct mechanisms of axonal globule formation in mice expressing human wild type α-synuclein or dementia with Lewy bodies-linked P123H ß-synuclein
title_fullStr Distinct mechanisms of axonal globule formation in mice expressing human wild type α-synuclein or dementia with Lewy bodies-linked P123H ß-synuclein
title_full_unstemmed Distinct mechanisms of axonal globule formation in mice expressing human wild type α-synuclein or dementia with Lewy bodies-linked P123H ß-synuclein
title_sort distinct mechanisms of axonal globule formation in mice expressing human wild type α-synuclein or dementia with lewy bodies-linked p123h ß-synuclein
publisher BMC
series Molecular Brain
issn 1756-6606
publishDate 2012-09-01
description <p>Abstract</p> <p>Background</p> <p>Axonopathy is critical in the early pathogenesis of neurodegenerative diseases, including Parkinson’s disease (PD) and dementia with Lewy bodies (DLB). Axonal swellings such as globules and spheroids are a distinct feature of axonopathy and our recent study showed that transgenic (tg) mice expressing DLB-linked P123H β-synuclein (P123H βS) were characterized by P123H βS-immunoreactive axonal swellings (P123H βS-globules). Therefore, the objectives of this study were to evaluate α-synuclein (αS)-immunoreactive axonal swellings (αS-globules) in the brains of tg mice expressing human wild-type αS and to compare them with the globules in P123H βS tg mice.</p> <p>Results</p> <p>In αS tg mice, αS-globules were formed in an age-dependent manner in various brain regions, including the thalamus and basal ganglia. These globules were composed of autophagosome-like membranous structures and were reminiscent of P123H βS-globules in P123H βS tg mice. In the αS-globules, frequent clustering and deformation of mitochondria were observed. These changes were associated with oxidative stress, based on staining of nitrated αS and 4-hydroxy-2-nonenal (4-HNE). In accord with the absence of mitochondria in the P123H βS-globules, staining of nitrated αS and 4-HNE in these globules was weaker than that for αS-globules. Leucine-rich repeat kinase 2 (LRRK2), the PARK8 of familial PD, was detected exclusively in αS-globules, suggesting a specific role of this molecule in these globules.</p> <p>Conclusions</p> <p>Lysosomal pathology was similarly observed for both αS- and P123H βS-globules, while oxidative stress was associated with the αS-globules, and to a lesser extent with the P123H βS-globules. Other pathologies, such as mitochondrial alteration and LRRK2 accumulation, were exclusively detected for αS-globules. Collectively, both αS- and P123H βS-globules were formed through similar but distinct pathogenic mechanisms. Our findings suggest that synuclein family members might contribute to diverse axonal pathologies.</p>
topic α-synuclein
P123H β-synuclein
Parkinson’s disease
Mitochondria
Lysosome
Transgenic mouse
url http://www.molecularbrain.com/content/5/1/34
work_keys_str_mv AT sekigawaakio distinctmechanismsofaxonalglobuleformationinmiceexpressinghumanwildtypeasynucleinordementiawithlewybodieslinkedp123hßsynuclein
AT fujitamasayo distinctmechanismsofaxonalglobuleformationinmiceexpressinghumanwildtypeasynucleinordementiawithlewybodieslinkedp123hßsynuclein
AT sekiyamakazunari distinctmechanismsofaxonalglobuleformationinmiceexpressinghumanwildtypeasynucleinordementiawithlewybodieslinkedp123hßsynuclein
AT takamatsuyoshiki distinctmechanismsofaxonalglobuleformationinmiceexpressinghumanwildtypeasynucleinordementiawithlewybodieslinkedp123hßsynuclein
AT hatanotaku distinctmechanismsofaxonalglobuleformationinmiceexpressinghumanwildtypeasynucleinordementiawithlewybodieslinkedp123hßsynuclein
AT rockensteinedward distinctmechanismsofaxonalglobuleformationinmiceexpressinghumanwildtypeasynucleinordementiawithlewybodieslinkedp123hßsynuclein
AT laspadaalbertr distinctmechanismsofaxonalglobuleformationinmiceexpressinghumanwildtypeasynucleinordementiawithlewybodieslinkedp123hßsynuclein
AT masliaheliezer distinctmechanismsofaxonalglobuleformationinmiceexpressinghumanwildtypeasynucleinordementiawithlewybodieslinkedp123hßsynuclein
AT hashimotomakoto distinctmechanismsofaxonalglobuleformationinmiceexpressinghumanwildtypeasynucleinordementiawithlewybodieslinkedp123hßsynuclein
_version_ 1725271806466588672

Similar Items