TSPO PET upregulation predicts epileptic phenotype at disease onset independently from chronic TSPO expression in a rat model of temporal lobe epilepsy

TSPO PET upregulation predicts epileptic phenotype at disease onset independently from chronic TSPO expression in a rat model of temporal lobe epilepsy

Neuroinflammation is a key component of epileptogenesis, the process leading to acquired epilepsy. In recent years, with the development of non-invasive in vivo positron emission tomography (PET) imaging of translocator protein 18 kDa (TSPO), a marker of neuroinflammation, it has become possible to...

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Main Authors: Daniele Bertoglio, Halima Amhaoul, Joery Goossens, Idrish Ali, Elisabeth Jonckers, Tom Bijnens, Matteo Siano, Leonie wyffels, Jeroen Verhaeghe, Annemie Van der Linden, Steven Staelens, Stefanie Dedeurwaerdere
Format: Article
Language:English
Published: Elsevier 2021-01-01
Series:NeuroImage: Clinical
Subjects:
Translocator protein
Inflammation
PET imaging
Neuroimaging
Kainic acid
KASE
Online Access:http://www.sciencedirect.com/science/article/pii/S2213158221001455
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spelling doaj-a00c894885164fe5bc81f163bc88c7432021-08-28T04:44:47ZengElsevierNeuroImage: Clinical2213-15822021-01-0131102701TSPO PET upregulation predicts epileptic phenotype at disease onset independently from chronic TSPO expression in a rat model of temporal lobe epilepsyDaniele Bertoglio0Halima Amhaoul1Joery Goossens2Idrish Ali3Elisabeth Jonckers4Tom Bijnens5Matteo Siano6Leonie wyffels7Jeroen Verhaeghe8Annemie Van der Linden9Steven Staelens10Stefanie Dedeurwaerdere11Molecular Imaging Center Antwerp, University of Antwerp, Belgium; Department of Translational Neurosciences, University of Antwerp, Belgium; Corresponding author at: Molecular Imaging Center Antwerp, University of Antwerp, Belgium.Department of Translational Neurosciences, University of Antwerp, BelgiumDepartment of Translational Neurosciences, University of Antwerp, BelgiumDepartment of Translational Neurosciences, University of Antwerp, BelgiumBio-Imaging Lab, University of Antwerp, BelgiumDepartment of Translational Neurosciences, University of Antwerp, BelgiumDepartment of Translational Neurosciences, University of Antwerp, BelgiumMolecular Imaging Center Antwerp, University of Antwerp, Belgium; Department of Nuclear Medicine, Antwerp University Hospital, Edegem, BelgiumMolecular Imaging Center Antwerp, University of Antwerp, BelgiumBio-Imaging Lab, University of Antwerp, BelgiumDepartment of Translational Neurosciences, University of Antwerp, BelgiumLaboratory of Experimental Hematology, University of Antwerp, BelgiumNeuroinflammation is a key component of epileptogenesis, the process leading to acquired epilepsy. In recent years, with the development of non-invasive in vivo positron emission tomography (PET) imaging of translocator protein 18 kDa (TSPO), a marker of neuroinflammation, it has become possible to perform longitudinal studies to characterize neuroinflammation at different disease stages in animal models of epileptogenesis. This study aimed to utilize the prognostic capability of TSPO PET imaging at disease onset (2 weeks post-SE) to categorize epileptic rats with distinct seizure burden based on TSPO levels at disease onset and investigate their association to TSPO expression at the chronic epilepsy stage. Controls (n = 14) and kainic acid-induced status epilepticus (KASE) rats (n = 41) were scanned non-invasively with [18F]PBR111 PET imaging measuring TSPO expression. Animals were monitored using video-electroencephalography (vEEG) up to chronic disease (12 weeks post-SE), at which TSPO levels ([3H]PK11195) as well as other post-mortem abnormalities (namely synaptic density ([3H]UCB-J), neuronal loss (NeuN), and neurodegeneration (FjC)) were investigated. By applying multivariate analysis, TSPO PET imaging at disease onset identified three KASE groups with significantly different spontaneous recurrent seizures (SRS) burden (defined as rare SRS, sporadic SRS, and frequent SRS) (p = 0.003). Interestingly, TSPO levels were significantly different when comparing the three KASE groups (p < 0.0001), with the frequent SRS group characterized only by a limited focal TSPO increase at disease onset. On the contrary, TSPO measured during chronic epilepsy was found to be the highest in the frequent SRS group and correlated with seizure burden (r = 0.826, p < 0.0001). Importantly, early and chronic TSPO levels did not correlate (r = −0.05). Finally, significant pathological changes in neuronal loss, synaptic density, and neurodegeneration were found not only when compared to control animals (p < 0.01), but also between the three KASE rat categories in the hippocampus (p < 0.05). Early and chronic TSPO upregulation following epileptogenic insult appear to be driven by two superimposed dynamic processes. The former is associated with epileptogenesis as measured at disease onset, while the latter is related to seizure frequency as quantified during chronic epilepsy.http://www.sciencedirect.com/science/article/pii/S2213158221001455Translocator proteinInflammationPET imagingNeuroimagingKainic acidKASE
collection DOAJ
language English
format Article
sources DOAJ
author Daniele Bertoglio
Halima Amhaoul
Joery Goossens
Idrish Ali
Elisabeth Jonckers
Tom Bijnens
Matteo Siano
Leonie wyffels
Jeroen Verhaeghe
Annemie Van der Linden
Steven Staelens
Stefanie Dedeurwaerdere
spellingShingle Daniele Bertoglio
Halima Amhaoul
Joery Goossens
Idrish Ali
Elisabeth Jonckers
Tom Bijnens
Matteo Siano
Leonie wyffels
Jeroen Verhaeghe
Annemie Van der Linden
Steven Staelens
Stefanie Dedeurwaerdere
TSPO PET upregulation predicts epileptic phenotype at disease onset independently from chronic TSPO expression in a rat model of temporal lobe epilepsy
NeuroImage: Clinical
Translocator protein
Inflammation
PET imaging
Neuroimaging
Kainic acid
KASE
author_facet Daniele Bertoglio
Halima Amhaoul
Joery Goossens
Idrish Ali
Elisabeth Jonckers
Tom Bijnens
Matteo Siano
Leonie wyffels
Jeroen Verhaeghe
Annemie Van der Linden
Steven Staelens
Stefanie Dedeurwaerdere
author_sort Daniele Bertoglio
title TSPO PET upregulation predicts epileptic phenotype at disease onset independently from chronic TSPO expression in a rat model of temporal lobe epilepsy
title_short TSPO PET upregulation predicts epileptic phenotype at disease onset independently from chronic TSPO expression in a rat model of temporal lobe epilepsy
title_full TSPO PET upregulation predicts epileptic phenotype at disease onset independently from chronic TSPO expression in a rat model of temporal lobe epilepsy
title_fullStr TSPO PET upregulation predicts epileptic phenotype at disease onset independently from chronic TSPO expression in a rat model of temporal lobe epilepsy
title_full_unstemmed TSPO PET upregulation predicts epileptic phenotype at disease onset independently from chronic TSPO expression in a rat model of temporal lobe epilepsy
title_sort tspo pet upregulation predicts epileptic phenotype at disease onset independently from chronic tspo expression in a rat model of temporal lobe epilepsy
publisher Elsevier
series NeuroImage: Clinical
issn 2213-1582
publishDate 2021-01-01
description Neuroinflammation is a key component of epileptogenesis, the process leading to acquired epilepsy. In recent years, with the development of non-invasive in vivo positron emission tomography (PET) imaging of translocator protein 18 kDa (TSPO), a marker of neuroinflammation, it has become possible to perform longitudinal studies to characterize neuroinflammation at different disease stages in animal models of epileptogenesis. This study aimed to utilize the prognostic capability of TSPO PET imaging at disease onset (2 weeks post-SE) to categorize epileptic rats with distinct seizure burden based on TSPO levels at disease onset and investigate their association to TSPO expression at the chronic epilepsy stage. Controls (n = 14) and kainic acid-induced status epilepticus (KASE) rats (n = 41) were scanned non-invasively with [18F]PBR111 PET imaging measuring TSPO expression. Animals were monitored using video-electroencephalography (vEEG) up to chronic disease (12 weeks post-SE), at which TSPO levels ([3H]PK11195) as well as other post-mortem abnormalities (namely synaptic density ([3H]UCB-J), neuronal loss (NeuN), and neurodegeneration (FjC)) were investigated. By applying multivariate analysis, TSPO PET imaging at disease onset identified three KASE groups with significantly different spontaneous recurrent seizures (SRS) burden (defined as rare SRS, sporadic SRS, and frequent SRS) (p = 0.003). Interestingly, TSPO levels were significantly different when comparing the three KASE groups (p < 0.0001), with the frequent SRS group characterized only by a limited focal TSPO increase at disease onset. On the contrary, TSPO measured during chronic epilepsy was found to be the highest in the frequent SRS group and correlated with seizure burden (r = 0.826, p < 0.0001). Importantly, early and chronic TSPO levels did not correlate (r = −0.05). Finally, significant pathological changes in neuronal loss, synaptic density, and neurodegeneration were found not only when compared to control animals (p < 0.01), but also between the three KASE rat categories in the hippocampus (p < 0.05). Early and chronic TSPO upregulation following epileptogenic insult appear to be driven by two superimposed dynamic processes. The former is associated with epileptogenesis as measured at disease onset, while the latter is related to seizure frequency as quantified during chronic epilepsy.
topic Translocator protein
Inflammation
PET imaging
Neuroimaging
Kainic acid
KASE
url http://www.sciencedirect.com/science/article/pii/S2213158221001455
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