Fundamentally different roles of neuronal TNF receptors in CNS pathology: TNFR1 and IKKβ promote microglial responses and tissue injury in demyelination while TNFR2 protects against excitotoxicity in mice

Fundamentally different roles of neuronal TNF receptors in CNS pathology: TNFR1 and IKKβ promote microglial responses and tissue injury in demyelination while TNFR2 protects against excitotoxicity in mice

Abstract Background During inflammatory demyelination, TNF receptor 1 (TNFR1) mediates detrimental proinflammatory effects of soluble TNF (solTNF), whereas TNFR2 mediates beneficial effects of transmembrane TNF (tmTNF) through oligodendroglia, microglia, and possibly other cell types. This model sup...

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Main Authors: Irini Papazian, Eleni Tsoukala, Athena Boutou, Maria Karamita, Konstantinos Kambas, Lida Iliopoulou, Roman Fischer, Roland E. Kontermann, Maria C. Denis, George Kollias, Hans Lassmann, Lesley Probert
Format: Article
Language:English
Published: BMC 2021-09-01
Series:Journal of Neuroinflammation
Subjects:
Neuroinflammation
Immunotherapy
Multiple sclerosis
NF-κB
Autophagy
Neuroprotection
Online Access:https://doi.org/10.1186/s12974-021-02200-4
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language English
format Article
sources DOAJ
author Irini Papazian
Eleni Tsoukala
Athena Boutou
Maria Karamita
Konstantinos Kambas
Lida Iliopoulou
Roman Fischer
Roland E. Kontermann
Maria C. Denis
George Kollias
Hans Lassmann
Lesley Probert
spellingShingle Irini Papazian
Eleni Tsoukala
Athena Boutou
Maria Karamita
Konstantinos Kambas
Lida Iliopoulou
Roman Fischer
Roland E. Kontermann
Maria C. Denis
George Kollias
Hans Lassmann
Lesley Probert
Fundamentally different roles of neuronal TNF receptors in CNS pathology: TNFR1 and IKKβ promote microglial responses and tissue injury in demyelination while TNFR2 protects against excitotoxicity in mice
Journal of Neuroinflammation
Neuroinflammation
Immunotherapy
Multiple sclerosis
NF-κB
Autophagy
Neuroprotection
author_facet Irini Papazian
Eleni Tsoukala
Athena Boutou
Maria Karamita
Konstantinos Kambas
Lida Iliopoulou
Roman Fischer
Roland E. Kontermann
Maria C. Denis
George Kollias
Hans Lassmann
Lesley Probert
author_sort Irini Papazian
title Fundamentally different roles of neuronal TNF receptors in CNS pathology: TNFR1 and IKKβ promote microglial responses and tissue injury in demyelination while TNFR2 protects against excitotoxicity in mice
title_short Fundamentally different roles of neuronal TNF receptors in CNS pathology: TNFR1 and IKKβ promote microglial responses and tissue injury in demyelination while TNFR2 protects against excitotoxicity in mice
title_full Fundamentally different roles of neuronal TNF receptors in CNS pathology: TNFR1 and IKKβ promote microglial responses and tissue injury in demyelination while TNFR2 protects against excitotoxicity in mice
title_fullStr Fundamentally different roles of neuronal TNF receptors in CNS pathology: TNFR1 and IKKβ promote microglial responses and tissue injury in demyelination while TNFR2 protects against excitotoxicity in mice
title_full_unstemmed Fundamentally different roles of neuronal TNF receptors in CNS pathology: TNFR1 and IKKβ promote microglial responses and tissue injury in demyelination while TNFR2 protects against excitotoxicity in mice
title_sort fundamentally different roles of neuronal tnf receptors in cns pathology: tnfr1 and ikkβ promote microglial responses and tissue injury in demyelination while tnfr2 protects against excitotoxicity in mice
publisher BMC
series Journal of Neuroinflammation
issn 1742-2094
publishDate 2021-09-01
description Abstract Background During inflammatory demyelination, TNF receptor 1 (TNFR1) mediates detrimental proinflammatory effects of soluble TNF (solTNF), whereas TNFR2 mediates beneficial effects of transmembrane TNF (tmTNF) through oligodendroglia, microglia, and possibly other cell types. This model supports the use of selective inhibitors of solTNF/TNFR1 as anti-inflammatory drugs for central nervous system (CNS) diseases. A potential obstacle is the neuroprotective effect of solTNF pretreatment described in cultured neurons, but the relevance in vivo is unknown. Methods To address this question, we generated mice with neuron-specific depletion of TNFR1, TNFR2, or inhibitor of NF-κB kinase subunit β (IKKβ), a main downstream mediator of TNFR signaling, and applied experimental models of inflammatory demyelination and acute and preconditioning glutamate excitotoxicity. We also investigated the molecular and cellular requirements of solTNF neuroprotection by generating astrocyte-neuron co-cultures with different combinations of wild-type (WT) and TNF and TNFR knockout cells and measuring N-methyl-d-aspartate (NMDA) excitotoxicity in vitro. Results Neither neuronal TNFR1 nor TNFR2 protected mice during inflammatory demyelination. In fact, both neuronal TNFR1 and neuronal IKKβ promoted microglial responses and tissue injury, and TNFR1 was further required for oligodendrocyte loss and axonal damage in cuprizone-induced demyelination. In contrast, neuronal TNFR2 increased preconditioning protection in a kainic acid (KA) excitotoxicity model in mice and limited hippocampal neuron death. The protective effects of neuronal TNFR2 observed in vivo were further investigated in vitro. As previously described, pretreatment of astrocyte-neuron co-cultures with solTNF (and therefore TNFR1) protected them against NMDA excitotoxicity. However, protection was dependent on astrocyte, not neuronal TNFR1, on astrocyte tmTNF-neuronal TNFR2 interactions, and was reproduced by a TNFR2 agonist. Conclusions These results demonstrate that neuronal TNF receptors perform fundamentally different roles in CNS pathology in vivo, with neuronal TNFR1 and IKKβ promoting microglial inflammation and neurotoxicity in demyelination, and neuronal TNFR2 mediating neuroprotection in excitotoxicity. They also reveal that previously described neuroprotective effects of solTNF against glutamate excitotoxicity in vitro are indirect and mediated via astrocyte tmTNF-neuron TNFR2 interactions. These results consolidate the concept that selective inhibition of solTNF/TNFR1 with maintenance of TNFR2 function would have combined anti-inflammatory and neuroprotective properties required for safe treatment of CNS diseases.
topic Neuroinflammation
Immunotherapy
Multiple sclerosis
NF-κB
Autophagy
Neuroprotection
url https://doi.org/10.1186/s12974-021-02200-4
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spelling doaj-f835375dd4814f7eb875ab3d9fd3f00f2021-09-26T11:49:55ZengBMCJournal of Neuroinflammation1742-20942021-09-0118112110.1186/s12974-021-02200-4Fundamentally different roles of neuronal TNF receptors in CNS pathology: TNFR1 and IKKβ promote microglial responses and tissue injury in demyelination while TNFR2 protects against excitotoxicity in miceIrini Papazian0Eleni Tsoukala1Athena Boutou2Maria Karamita3Konstantinos Kambas4Lida Iliopoulou5Roman Fischer6Roland E. Kontermann7Maria C. Denis8George Kollias9Hans Lassmann10Lesley Probert11Laboratory of Molecular Genetics, Department of Immunology, Hellenic Pasteur InstituteLaboratory of Molecular Genetics, Department of Immunology, Hellenic Pasteur InstituteLaboratory of Molecular Genetics, Department of Immunology, Hellenic Pasteur InstituteLaboratory of Molecular Genetics, Department of Immunology, Hellenic Pasteur InstituteLaboratory of Molecular Genetics, Department of Immunology, Hellenic Pasteur InstituteLaboratory of Molecular Genetics, Department of Immunology, Hellenic Pasteur InstituteInstitute of Cell Biology and Immunology, University of StuttgartInstitute of Cell Biology and Immunology, University of StuttgartInstitute of Immunology, Biomedical Sciences Research Centre (BSRC) “Alexander Fleming”Institute of Immunology, Biomedical Sciences Research Centre (BSRC) “Alexander Fleming”Department of Neuroimmunology, Center for Brain Research, Medical University of ViennaLaboratory of Molecular Genetics, Department of Immunology, Hellenic Pasteur InstituteAbstract Background During inflammatory demyelination, TNF receptor 1 (TNFR1) mediates detrimental proinflammatory effects of soluble TNF (solTNF), whereas TNFR2 mediates beneficial effects of transmembrane TNF (tmTNF) through oligodendroglia, microglia, and possibly other cell types. This model supports the use of selective inhibitors of solTNF/TNFR1 as anti-inflammatory drugs for central nervous system (CNS) diseases. A potential obstacle is the neuroprotective effect of solTNF pretreatment described in cultured neurons, but the relevance in vivo is unknown. Methods To address this question, we generated mice with neuron-specific depletion of TNFR1, TNFR2, or inhibitor of NF-κB kinase subunit β (IKKβ), a main downstream mediator of TNFR signaling, and applied experimental models of inflammatory demyelination and acute and preconditioning glutamate excitotoxicity. We also investigated the molecular and cellular requirements of solTNF neuroprotection by generating astrocyte-neuron co-cultures with different combinations of wild-type (WT) and TNF and TNFR knockout cells and measuring N-methyl-d-aspartate (NMDA) excitotoxicity in vitro. Results Neither neuronal TNFR1 nor TNFR2 protected mice during inflammatory demyelination. In fact, both neuronal TNFR1 and neuronal IKKβ promoted microglial responses and tissue injury, and TNFR1 was further required for oligodendrocyte loss and axonal damage in cuprizone-induced demyelination. In contrast, neuronal TNFR2 increased preconditioning protection in a kainic acid (KA) excitotoxicity model in mice and limited hippocampal neuron death. The protective effects of neuronal TNFR2 observed in vivo were further investigated in vitro. As previously described, pretreatment of astrocyte-neuron co-cultures with solTNF (and therefore TNFR1) protected them against NMDA excitotoxicity. However, protection was dependent on astrocyte, not neuronal TNFR1, on astrocyte tmTNF-neuronal TNFR2 interactions, and was reproduced by a TNFR2 agonist. Conclusions These results demonstrate that neuronal TNF receptors perform fundamentally different roles in CNS pathology in vivo, with neuronal TNFR1 and IKKβ promoting microglial inflammation and neurotoxicity in demyelination, and neuronal TNFR2 mediating neuroprotection in excitotoxicity. They also reveal that previously described neuroprotective effects of solTNF against glutamate excitotoxicity in vitro are indirect and mediated via astrocyte tmTNF-neuron TNFR2 interactions. These results consolidate the concept that selective inhibition of solTNF/TNFR1 with maintenance of TNFR2 function would have combined anti-inflammatory and neuroprotective properties required for safe treatment of CNS diseases.https://doi.org/10.1186/s12974-021-02200-4NeuroinflammationImmunotherapyMultiple sclerosisNF-κBAutophagyNeuroprotection

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