Expression of neurodegenerative disease-related proteins and caspase-3 in glioneuronal tumours

Aims Recent evidence supports the activation of mechanisms underlying cellular ageing and neurodegeneration in developmental lesions associated with epilepsy. The present study examined the ongoing cell injury and vulnerability to neuronal degeneration in glioneuronal tumours (GNT). Methods We evalu...

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Published inNeuropathology and applied neurobiology Vol. 41; no. 2; pp. e1 - e15
Main Authors Prabowo, A. S., Iyer, A. M., Veersema, T. J., Anink, J. J., Schouten-van Meeteren, A. Y. N., Spliet, W. G. M., van Rijen, P. C., Ferrier, C. H., Thom, M., Aronica, E.
Format Journal Article
LanguageEnglish
Published England Blackwell Publishing Ltd 01.02.2015
Wiley Subscription Services, Inc
Subjects
Adolescent
Adult
apoptosis
Biomarkers, Tumor - analysis
Caspase 3 - analysis
Caspase 3 - biosynthesis
Child
Epilepsy
Epilepsy - etiology
Female
Ganglioglioma - complications
Ganglioglioma - metabolism
Humans
Immunohistochemistry
long-term epilepsy-associated tumours
Male
mTOR
Nerve Degeneration - complications
Nerve Degeneration - metabolism
Neurodegeneration
Neuroectodermal Tumors, Primitive - complications
Neuroectodermal Tumors, Primitive - metabolism
Tumors
epilepsy
mTOR
neurodegeneration
apoptosis
long-term epilepsy-associated tumours
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Abstract Aims Recent evidence supports the activation of mechanisms underlying cellular ageing and neurodegeneration in developmental lesions associated with epilepsy. The present study examined the ongoing cell injury and vulnerability to neuronal degeneration in glioneuronal tumours (GNT). Methods We evaluated a series of GNT (n = 31 gangliogliomas, GG and n = 30 dysembryoplastic neuroepithelial tumours, DNT). Sections were processed for immunohistochemistry using markers for the evaluation of caspase‐3 and neurodegeneration‐related proteins/pathways and their expression was correlated with the tumour features and the clinical history of epilepsy. Results Both GG and DNT specimens contained caspase‐3‐positive cells. In GG, expression of activated caspase‐3 was negatively correlated the with the BRAF V600E mutation status. We also observed an abnormal expression of death receptor‐6 and β‐amyloid precursor protein (APP). Moreover, dysplastic neurones expressed p62, phosphorylated (p)TDP43 and pTau. Double labelling experiments showed colocalization of phosphorylated S6 (marker of mammalian target of rapamycin, mTOR, pathway activation) with pTau and p62. In GG, neuronal p62 expression was positively correlated with pS6. The immunoreactivity score (IRS) of caspase‐3, APP, DR6, p62 and pTDP43 were found to be significantly higher in GG than in DNT. Expression of APP, DR6, pTau (in GG and DNT) and caspase‐3 (in GG) positively correlated with duration of epilepsy. In GG, the expression of neuronal caspase‐3, DR6 and glial p62 was associated with a worse postoperative seizure outcome. Conclusions Our observations in GNT provide evidence of premature activation of mechanisms of neurodegeneration which are associated with the clinical course of epilepsy in patient with GG.
AbstractList AIMSRecent evidence supports the activation of mechanisms underlying cellular ageing and neurodegeneration in developmental lesions associated with epilepsy. The present study examined the ongoing cell injury and vulnerability to neuronal degeneration in glioneuronal tumours (GNT).METHODSWe evaluated a series of GNT (n = 31 gangliogliomas, GG and n = 30 dysembryoplastic neuroepithelial tumours, DNT). Sections were processed for immunohistochemistry using markers for the evaluation of caspase-3 and neurodegeneration-related proteins/pathways and their expression was correlated with the tumour features and the clinical history of epilepsy.RESULTSBoth GG and DNT specimens contained caspase-3-positive cells. In GG, expression of activated caspase-3 was negatively correlated the with the BRAF V600E mutation status. We also observed an abnormal expression of death receptor-6 and β-amyloid precursor protein (APP). Moreover, dysplastic neurones expressed p62, phosphorylated (p)TDP43 and pTau. Double labelling experiments showed colocalization of phosphorylated S6 (marker of mammalian target of rapamycin, mTOR, pathway activation) with pTau and p62. In GG, neuronal p62 expression was positively correlated with pS6. The immunoreactivity score (IRS) of caspase-3, APP, DR6, p62 and pTDP43 were found to be significantly higher in GG than in DNT. Expression of APP, DR6, pTau (in GG and DNT) and caspase-3 (in GG) positively correlated with duration of epilepsy. In GG, the expression of neuronal caspase-3, DR6 and glial p62 was associated with a worse postoperative seizure outcome.CONCLUSIONSOur observations in GNT provide evidence of premature activation of mechanisms of neurodegeneration which are associated with the clinical course of epilepsy in patient with GG.
Aims Recent evidence supports the activation of mechanisms underlying cellular ageing and neurodegeneration in developmental lesions associated with epilepsy. The present study examined the ongoing cell injury and vulnerability to neuronal degeneration in glioneuronal tumours (GNT). Methods We evaluated a series of GNT (n=31 gangliogliomas, GG and n=30 dysembryoplastic neuroepithelial tumours, DNT). Sections were processed for immunohistochemistry using markers for the evaluation of caspase-3 and neurodegeneration-related proteins/pathways and their expression was correlated with the tumour features and the clinical history of epilepsy. Results Both GG and DNT specimens contained caspase-3-positive cells. In GG, expression of activated caspase-3 was negatively correlated the with the BRAF V600E mutation status. We also observed an abnormal expression of death receptor-6 and [beta]-amyloid precursor protein (APP). Moreover, dysplastic neurones expressed p62, phosphorylated (p)TDP43 and pTau. Double labelling experiments showed colocalization of phosphorylated S6 (marker of mammalian target of rapamycin, mTOR, pathway activation) with pTau and p62. In GG, neuronal p62 expression was positively correlated with pS6. The immunoreactivity score (IRS) of caspase-3, APP, DR6, p62 and pTDP43 were found to be significantly higher in GG than in DNT. Expression of APP, DR6, pTau (in GG and DNT) and caspase-3 (in GG) positively correlated with duration of epilepsy. In GG, the expression of neuronal caspase-3, DR6 and glial p62 was associated with a worse postoperative seizure outcome. Conclusions Our observations in GNT provide evidence of premature activation of mechanisms of neurodegeneration which are associated with the clinical course of epilepsy in patient with GG.
Aims Recent evidence supports the activation of mechanisms underlying cellular ageing and neurodegeneration in developmental lesions associated with epilepsy. The present study examined the ongoing cell injury and vulnerability to neuronal degeneration in glioneuronal tumours ( GNT ). Methods We evaluated a series of GNT ( n  = 31 gangliogliomas, GG and n  = 30 dysembryoplastic neuroepithelial tumours, DNT ). Sections were processed for immunohistochemistry using markers for the evaluation of caspase‐3 and neurodegeneration‐related proteins/pathways and their expression was correlated with the tumour features and the clinical history of epilepsy. Results Both GG and DNT specimens contained caspase‐3‐positive cells. In GG , expression of activated caspase‐3 was negatively correlated the with the BRAF V 600 E mutation status. We also observed an abnormal expression of death receptor‐6 and β‐amyloid precursor protein ( APP ). Moreover, dysplastic neurones expressed p62, phosphorylated (p) TDP 43 and pTau . Double labelling experiments showed colocalization of phosphorylated S 6 (marker of mammalian target of rapamycin, mTOR , pathway activation) with pTau and p62. In GG , neuronal p62 expression was positively correlated with pS 6. The immunoreactivity score ( IRS ) of caspase‐3, APP , DR 6, p62 and pTDP 43 were found to be significantly higher in GG than in DNT . Expression of APP , DR 6, pTau (in GG and DNT ) and caspase‐3 (in GG ) positively correlated with duration of epilepsy. In GG , the expression of neuronal caspase‐3, DR 6 and glial p62 was associated with a worse postoperative seizure outcome. Conclusions Our observations in GNT provide evidence of premature activation of mechanisms of neurodegeneration which are associated with the clinical course of epilepsy in patient with GG .
Aims Recent evidence supports the activation of mechanisms underlying cellular ageing and neurodegeneration in developmental lesions associated with epilepsy. The present study examined the ongoing cell injury and vulnerability to neuronal degeneration in glioneuronal tumours (GNT). Methods We evaluated a series of GNT (n = 31 gangliogliomas, GG and n = 30 dysembryoplastic neuroepithelial tumours, DNT). Sections were processed for immunohistochemistry using markers for the evaluation of caspase‐3 and neurodegeneration‐related proteins/pathways and their expression was correlated with the tumour features and the clinical history of epilepsy. Results Both GG and DNT specimens contained caspase‐3‐positive cells. In GG, expression of activated caspase‐3 was negatively correlated the with the BRAF V600E mutation status. We also observed an abnormal expression of death receptor‐6 and β‐amyloid precursor protein (APP). Moreover, dysplastic neurones expressed p62, phosphorylated (p)TDP43 and pTau. Double labelling experiments showed colocalization of phosphorylated S6 (marker of mammalian target of rapamycin, mTOR, pathway activation) with pTau and p62. In GG, neuronal p62 expression was positively correlated with pS6. The immunoreactivity score (IRS) of caspase‐3, APP, DR6, p62 and pTDP43 were found to be significantly higher in GG than in DNT. Expression of APP, DR6, pTau (in GG and DNT) and caspase‐3 (in GG) positively correlated with duration of epilepsy. In GG, the expression of neuronal caspase‐3, DR6 and glial p62 was associated with a worse postoperative seizure outcome. Conclusions Our observations in GNT provide evidence of premature activation of mechanisms of neurodegeneration which are associated with the clinical course of epilepsy in patient with GG.
Recent evidence supports the activation of mechanisms underlying cellular ageing and neurodegeneration in developmental lesions associated with epilepsy. The present study examined the ongoing cell injury and vulnerability to neuronal degeneration in glioneuronal tumours (GNT). We evaluated a series of GNT (n = 31 gangliogliomas, GG and n = 30 dysembryoplastic neuroepithelial tumours, DNT). Sections were processed for immunohistochemistry using markers for the evaluation of caspase-3 and neurodegeneration-related proteins/pathways and their expression was correlated with the tumour features and the clinical history of epilepsy. Both GG and DNT specimens contained caspase-3-positive cells. In GG, expression of activated caspase-3 was negatively correlated the with the BRAF V600E mutation status. We also observed an abnormal expression of death receptor-6 and β-amyloid precursor protein (APP). Moreover, dysplastic neurones expressed p62, phosphorylated (p)TDP43 and pTau. Double labelling experiments showed colocalization of phosphorylated S6 (marker of mammalian target of rapamycin, mTOR, pathway activation) with pTau and p62. In GG, neuronal p62 expression was positively correlated with pS6. The immunoreactivity score (IRS) of caspase-3, APP, DR6, p62 and pTDP43 were found to be significantly higher in GG than in DNT. Expression of APP, DR6, pTau (in GG and DNT) and caspase-3 (in GG) positively correlated with duration of epilepsy. In GG, the expression of neuronal caspase-3, DR6 and glial p62 was associated with a worse postoperative seizure outcome. Our observations in GNT provide evidence of premature activation of mechanisms of neurodegeneration which are associated with the clinical course of epilepsy in patient with GG.
Author Ferrier, C. H.
Prabowo, A. S.
Spliet, W. G. M.
Veersema, T. J.
Aronica, E.
Anink, J. J.
Iyer, A. M.
Schouten-van Meeteren, A. Y. N.
Thom, M.
van Rijen, P. C.
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Keywords epilepsy
mTOR
neurodegeneration
apoptosis
long-term epilepsy-associated tumours
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  year: 2015
  text: 2015-02
PublicationDecade 2010
PublicationPlace England
PublicationPlace_xml – name: England
– name: Oxford
PublicationTitle Neuropathology and applied neurobiology
PublicationTitleAlternate Neuropathol Appl Neurobiol
PublicationYear 2015
Publisher Blackwell Publishing Ltd
Wiley Subscription Services, Inc
Publisher_xml – name: Blackwell Publishing Ltd
– name: Wiley Subscription Services, Inc
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2012; 287
2013; 23
2010; 17
2013; 126
2013; 20
2003; 14
2013; 125
2014; 24
2002; 512
2003; 18
2008; 31
2011; 17
2008; 1
2013; 5
2012; 12
2012; 97
2001; 43
2009; 11
2004; 30
2010; 20
2012; 135
2006; 65
2013; 13
2011; 70
2005; 31
1999; 11
1999; 97
2009; 284
2008; 113
2009; 647
2012; 22
2012; 66
2010; 30
2012; 217
2010; 7
2014; 11
2011; 122
2008; 151
2011; 121
2003; 44
2012 Feb; 17
2011; 286
2003 Sep; 23
2010; 32
2014; 269C
2012; 102
2005; 115
2011; 30
2007
2011; 76
2010; 285
2006; 3
1993
1993; 90
2011; 37
2012; 149
2007; 55
2009; 457
2012; 109
2012; 50
2004; 10
2012; 90
2013; 36
1990; 26
2000; 74
2012 Jul; 393
2009; 6
1999; 30
2013; 252
2013
2012 May; 22
2012; 7
2008; 131
2012; 44
2007; 48
2012; 9
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Snippet Aims Recent evidence supports the activation of mechanisms underlying cellular ageing and neurodegeneration in developmental lesions associated with epilepsy....
Recent evidence supports the activation of mechanisms underlying cellular ageing and neurodegeneration in developmental lesions associated with epilepsy. The...
Aims Recent evidence supports the activation of mechanisms underlying cellular ageing and neurodegeneration in developmental lesions associated with epilepsy....
AIMSRecent evidence supports the activation of mechanisms underlying cellular ageing and neurodegeneration in developmental lesions associated with epilepsy....
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SubjectTerms Adolescent
Adult
apoptosis
Biomarkers, Tumor - analysis
Caspase 3 - analysis
Caspase 3 - biosynthesis
Child
Epilepsy
Epilepsy - etiology
Female
Ganglioglioma - complications
Ganglioglioma - metabolism
Humans
Immunohistochemistry
long-term epilepsy-associated tumours
Male
mTOR
Nerve Degeneration - complications
Nerve Degeneration - metabolism
Neurodegeneration
Neuroectodermal Tumors, Primitive - complications
Neuroectodermal Tumors, Primitive - metabolism
Tumors
Title Expression of neurodegenerative disease-related proteins and caspase-3 in glioneuronal tumours
URI https://api.istex.fr/ark:/67375/WNG-VBRRKD6N-X/fulltext.pdf
https://onlinelibrary.wiley.com/doi/abs/10.1111%2Fnan.12143
https://www.ncbi.nlm.nih.gov/pubmed/24750067
https://www.proquest.com/docview/1648869960/abstract/
https://search.proquest.com/docview/1652427904
Volume 41
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