Expression of Translocator Protein and [18F]-GE180 Ligand Uptake in Multiple Sclerosis Animal Models

Positron emission tomography (PET) ligands targeting the translocator protein (TSPO) represent promising tools to visualize neuroinflammation in multiple sclerosis (MS). Although it is known that TSPO is expressed in the outer mitochondria membrane, its cellular localization in the central nervous s...

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Autores principales: Nack, Anne, Brendel, Matthias, Nedelcu, Julia, Daerr, Markus, Nyamoya, Stella, Beyer, Cordian, Focke, Carola, Deussing, Maximilian, Hoornaert, Chloé, Ponsaerts, Peter, Schmitz, Christoph, Bartenstein, Peter, Rominger, Axel, Kipp, Markus
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2019
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6406715/
https://www.ncbi.nlm.nih.gov/pubmed/30696113
http://dx.doi.org/10.3390/cells8020094
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author Nack, Anne
Brendel, Matthias
Nedelcu, Julia
Daerr, Markus
Nyamoya, Stella
Beyer, Cordian
Focke, Carola
Deussing, Maximilian
Hoornaert, Chloé
Ponsaerts, Peter
Schmitz, Christoph
Bartenstein, Peter
Rominger, Axel
Kipp, Markus
author_facet Nack, Anne
Brendel, Matthias
Nedelcu, Julia
Daerr, Markus
Nyamoya, Stella
Beyer, Cordian
Focke, Carola
Deussing, Maximilian
Hoornaert, Chloé
Ponsaerts, Peter
Schmitz, Christoph
Bartenstein, Peter
Rominger, Axel
Kipp, Markus
author_sort Nack, Anne
collection PubMed
description Positron emission tomography (PET) ligands targeting the translocator protein (TSPO) represent promising tools to visualize neuroinflammation in multiple sclerosis (MS). Although it is known that TSPO is expressed in the outer mitochondria membrane, its cellular localization in the central nervous system under physiological and pathological conditions is not entirely clear. The purpose of this study was to assess the feasibility of utilizing PET imaging with the TSPO tracer, [18F]-GE180, to detect histopathological changes during experimental demyelination, and to determine which cell types express TSPO. C57BL/6 mice were fed with cuprizone for up to 5 weeks to induce demyelination. Groups of mice were investigated by [18F]-GE180 PET imaging at week 5. Recruitment of peripheral immune cells was triggered by combining cuprizone intoxication with MOG(35–55) immunization (i.e., Cup/EAE). Immunofluorescence double-labelling and transgene mice were used to determine which cell types express TSPO. [18F]-GE180-PET reliably detected the cuprizone-induced pathology in various white and grey matter regions, including the corpus callosum, cortex, hippocampus, thalamus and caudoputamen. Cuprizone-induced demyelination was paralleled by an increase in TSPO expression, glia activation and axonal injury. Most of the microglia and around one-third of the astrocytes expressed TSPO. TSPO expression induction was more severe in the white matter corpus callosum compared to the grey matter cortex. Although mitochondria accumulate at sites of focal axonal injury, these mitochondria do not express TSPO. In Cup/EAE mice, both microglia and recruited monocytes contribute to the TSPO expressing cell populations. These findings support the notion that TSPO is a valuable marker for the in vivo visualization and quantification of neuropathological changes in the MS brain. The pathological substrate of an increase in TSPO-ligand binding might be diverse including microglia activation, peripheral monocyte recruitment, or astrocytosis, but not axonal injury.
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spelling pubmed-64067152019-03-19 Expression of Translocator Protein and [18F]-GE180 Ligand Uptake in Multiple Sclerosis Animal Models Nack, Anne Brendel, Matthias Nedelcu, Julia Daerr, Markus Nyamoya, Stella Beyer, Cordian Focke, Carola Deussing, Maximilian Hoornaert, Chloé Ponsaerts, Peter Schmitz, Christoph Bartenstein, Peter Rominger, Axel Kipp, Markus Cells Article Positron emission tomography (PET) ligands targeting the translocator protein (TSPO) represent promising tools to visualize neuroinflammation in multiple sclerosis (MS). Although it is known that TSPO is expressed in the outer mitochondria membrane, its cellular localization in the central nervous system under physiological and pathological conditions is not entirely clear. The purpose of this study was to assess the feasibility of utilizing PET imaging with the TSPO tracer, [18F]-GE180, to detect histopathological changes during experimental demyelination, and to determine which cell types express TSPO. C57BL/6 mice were fed with cuprizone for up to 5 weeks to induce demyelination. Groups of mice were investigated by [18F]-GE180 PET imaging at week 5. Recruitment of peripheral immune cells was triggered by combining cuprizone intoxication with MOG(35–55) immunization (i.e., Cup/EAE). Immunofluorescence double-labelling and transgene mice were used to determine which cell types express TSPO. [18F]-GE180-PET reliably detected the cuprizone-induced pathology in various white and grey matter regions, including the corpus callosum, cortex, hippocampus, thalamus and caudoputamen. Cuprizone-induced demyelination was paralleled by an increase in TSPO expression, glia activation and axonal injury. Most of the microglia and around one-third of the astrocytes expressed TSPO. TSPO expression induction was more severe in the white matter corpus callosum compared to the grey matter cortex. Although mitochondria accumulate at sites of focal axonal injury, these mitochondria do not express TSPO. In Cup/EAE mice, both microglia and recruited monocytes contribute to the TSPO expressing cell populations. These findings support the notion that TSPO is a valuable marker for the in vivo visualization and quantification of neuropathological changes in the MS brain. The pathological substrate of an increase in TSPO-ligand binding might be diverse including microglia activation, peripheral monocyte recruitment, or astrocytosis, but not axonal injury. MDPI 2019-01-28 /pmc/articles/PMC6406715/ /pubmed/30696113 http://dx.doi.org/10.3390/cells8020094 Text en © 2019 by the authors. Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Nack, Anne
Brendel, Matthias
Nedelcu, Julia
Daerr, Markus
Nyamoya, Stella
Beyer, Cordian
Focke, Carola
Deussing, Maximilian
Hoornaert, Chloé
Ponsaerts, Peter
Schmitz, Christoph
Bartenstein, Peter
Rominger, Axel
Kipp, Markus
Expression of Translocator Protein and [18F]-GE180 Ligand Uptake in Multiple Sclerosis Animal Models
title Expression of Translocator Protein and [18F]-GE180 Ligand Uptake in Multiple Sclerosis Animal Models
title_full Expression of Translocator Protein and [18F]-GE180 Ligand Uptake in Multiple Sclerosis Animal Models
title_fullStr Expression of Translocator Protein and [18F]-GE180 Ligand Uptake in Multiple Sclerosis Animal Models
title_full_unstemmed Expression of Translocator Protein and [18F]-GE180 Ligand Uptake in Multiple Sclerosis Animal Models
title_short Expression of Translocator Protein and [18F]-GE180 Ligand Uptake in Multiple Sclerosis Animal Models
title_sort expression of translocator protein and [18f]-ge180 ligand uptake in multiple sclerosis animal models
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6406715/
https://www.ncbi.nlm.nih.gov/pubmed/30696113
http://dx.doi.org/10.3390/cells8020094
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