Astroglial modulation of synaptic function in the non-demyelinated cerebellar cortex is dependent on MyD88 signaling in a model of toxic demyelination

Melanie Lohrberg; Lena Sünke Mortensen; Carolina Thomas; Franziska Fries; Franziska van der Meer; Alexander Götz; Carolin Landt; Hong Jun Rhee; JeongSeop Rhee; David Gómez-Varela; Manuela Schmidt; Wiebke Möbius; Torben Ruhwedel; Luis A Pardo; Linus Remling; Nadine Kramann; Claudia Wrzos; Erik Bahn; Christine Stadelmann; Alonso Barrantes-Freer

doi:10.1186/s12974-025-03368-9

Astroglial modulation of synaptic function in the non-demyelinated cerebellar cortex is dependent on MyD88 signaling in a model of toxic demyelination

Melanie Lohrberg
, Lena Sünke Mortensen
, Carolina Thomas
, Franziska Fries
, Franziska van der Meer
, Alexander Götz
, Carolin Landt
, Hong Jun Rhee
, JeongSeop Rhee
, David Gómez-Varela
, Manuela Schmidt
, Wiebke Möbius
, Torben Ruhwedel
, Luis A Pardo
, Linus Remling
, Nadine Kramann
, Claudia Wrzos
, Erik Bahn
, Christine Stadelmann (Corresponding author)
, Alonso Barrantes-Freer (Corresponding author)

Department of Pharmaceutical Sciences

Publications: Contribution to journal › Article › Peer Reviewed

Abstract

Progressive neurological decline in multiple sclerosis is associated with axonal loss and synaptic dysfunction in the non-demyelinated normal appearing gray matter (NAGM) and prominently in the cerebellum. In contrast to early disease stages, where synaptic and neuro-axonal pathology correlates with the extent of T cell infiltration, a prominent role of the innate immune system has been proposed for progressive MS. However, the specific contribution of microglia and astrocytes to synaptic cerebellar pathology in the NAGM- independent of an adaptive T cell response - remains largely unexplored. In the present study, we quantified synaptic changes in the cerebellar NAGM distant from demyelinated lesions in a mouse model of toxic demyelination. Proteomic analysis of the cerebellar cortex revealed differential regulation of synaptic and glutamate transport proteins in the absence of evident structural synaptic pathology or local gray matter demyelination. At the functional level, synaptic changes manifested as a reduction in frequency-dependent facilitation at the parallel fiber- Purkinje cell synapse. Further, deficiency of MyD88, an adaptor protein of the innate immune response, associated with a functional recovery in facilitation, reduced changes in the differential expression of synaptic and glutamate transport proteins, and reduced transcription levels of inflammatory cytokines. Nevertheless, the characteristics of demyelinating lesions and their associated cellular response were similar to wild type animals. Our work brings forward an experimental paradigm mimicking the diffuse synaptic pathology independent of demyelination in late stage MS and highlights the complex regulation of synaptic pathology in the cerebellar NAGM. Moreover, our findings suggest a role of astrocytes, in particular Bergmann glia, as key cellular determinants of cerebellar synaptic dysfunction.

Original language	English
Article number	47
Number of pages	17
Journal	Journal of Neuroinflammation
Volume	22
Issue number	1
DOIs	https://doi.org/10.1186/s12974-025-03368-9
Publication status	Published - 23 Feb 2025

Austrian Fields of Science 2012

301405 Neuropathology

Keywords

Animals
Mice
Astrocytes/metabolism
Signal Transduction/physiology
Disease Models, Animal
Synapses/metabolism
Cerebellar Cortex/pathology
Myeloid Differentiation Factor 88/metabolism
Mice, Inbred C57BL
Demyelinating Diseases/pathology
Mice, Knockout
Cuprizone/toxicity
Male

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Cite this

Lohrberg, M., Mortensen, L. S., Thomas, C., Fries, F., van der Meer, F., Götz, A., Landt, C., Rhee, H. J., Rhee, J., Gómez-Varela, D., Schmidt, M., Möbius, W., Ruhwedel, T., Pardo, L. A., Remling, L., Kramann, N., Wrzos, C., Bahn, E., Stadelmann, C., & Barrantes-Freer, A. (2025). Astroglial modulation of synaptic function in the non-demyelinated cerebellar cortex is dependent on MyD88 signaling in a model of toxic demyelination. Journal of Neuroinflammation, 22(1), Article 47. https://doi.org/10.1186/s12974-025-03368-9

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title = "Astroglial modulation of synaptic function in the non-demyelinated cerebellar cortex is dependent on MyD88 signaling in a model of toxic demyelination",

abstract = "Progressive neurological decline in multiple sclerosis is associated with axonal loss and synaptic dysfunction in the non-demyelinated normal appearing gray matter (NAGM) and prominently in the cerebellum. In contrast to early disease stages, where synaptic and neuro-axonal pathology correlates with the extent of T cell infiltration, a prominent role of the innate immune system has been proposed for progressive MS. However, the specific contribution of microglia and astrocytes to synaptic cerebellar pathology in the NAGM- independent of an adaptive T cell response - remains largely unexplored. In the present study, we quantified synaptic changes in the cerebellar NAGM distant from demyelinated lesions in a mouse model of toxic demyelination. Proteomic analysis of the cerebellar cortex revealed differential regulation of synaptic and glutamate transport proteins in the absence of evident structural synaptic pathology or local gray matter demyelination. At the functional level, synaptic changes manifested as a reduction in frequency-dependent facilitation at the parallel fiber- Purkinje cell synapse. Further, deficiency of MyD88, an adaptor protein of the innate immune response, associated with a functional recovery in facilitation, reduced changes in the differential expression of synaptic and glutamate transport proteins, and reduced transcription levels of inflammatory cytokines. Nevertheless, the characteristics of demyelinating lesions and their associated cellular response were similar to wild type animals. Our work brings forward an experimental paradigm mimicking the diffuse synaptic pathology independent of demyelination in late stage MS and highlights the complex regulation of synaptic pathology in the cerebellar NAGM. Moreover, our findings suggest a role of astrocytes, in particular Bergmann glia, as key cellular determinants of cerebellar synaptic dysfunction.",

keywords = "Animals, Mice, Astrocytes/metabolism, Signal Transduction/physiology, Disease Models, Animal, Synapses/metabolism, Cerebellar Cortex/pathology, Myeloid Differentiation Factor 88/metabolism, Mice, Inbred C57BL, Demyelinating Diseases/pathology, Mice, Knockout, Cuprizone/toxicity, Male",

author = "Melanie Lohrberg and Mortensen, \{Lena S{\"u}nke\} and Carolina Thomas and Franziska Fries and \{van der Meer\}, Franziska and Alexander G{\"o}tz and Carolin Landt and Rhee, \{Hong Jun\} and JeongSeop Rhee and David G{\'o}mez-Varela and Manuela Schmidt and Wiebke M{\"o}bius and Torben Ruhwedel and Pardo, \{Luis A\} and Linus Remling and Nadine Kramann and Claudia Wrzos and Erik Bahn and Christine Stadelmann and Alonso Barrantes-Freer",

note = "{\textcopyright} 2025. The Author(s).",

year = "2025",

month = feb,

day = "23",

doi = "10.1186/s12974-025-03368-9",

language = "English",

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Lohrberg, M, Mortensen, LS, Thomas, C, Fries, F, van der Meer, F, Götz, A, Landt, C, Rhee, HJ, Rhee, J, Gómez-Varela, D , Schmidt, M, Möbius, W, Ruhwedel, T, Pardo, LA, Remling, L, Kramann, N, Wrzos, C, Bahn, E, Stadelmann, C & Barrantes-Freer, A 2025, 'Astroglial modulation of synaptic function in the non-demyelinated cerebellar cortex is dependent on MyD88 signaling in a model of toxic demyelination', Journal of Neuroinflammation, vol. 22, no. 1, 47. https://doi.org/10.1186/s12974-025-03368-9

TY - JOUR

T1 - Astroglial modulation of synaptic function in the non-demyelinated cerebellar cortex is dependent on MyD88 signaling in a model of toxic demyelination

AU - Lohrberg, Melanie

AU - Mortensen, Lena Sünke

AU - Thomas, Carolina

AU - Fries, Franziska

AU - van der Meer, Franziska

AU - Götz, Alexander

AU - Landt, Carolin

AU - Rhee, Hong Jun

AU - Rhee, JeongSeop

AU - Gómez-Varela, David

AU - Schmidt, Manuela

AU - Möbius, Wiebke

AU - Ruhwedel, Torben

AU - Pardo, Luis A

AU - Remling, Linus

AU - Kramann, Nadine

AU - Wrzos, Claudia

AU - Bahn, Erik

AU - Stadelmann, Christine

AU - Barrantes-Freer, Alonso

PY - 2025/2/23

Y1 - 2025/2/23

N2 - Progressive neurological decline in multiple sclerosis is associated with axonal loss and synaptic dysfunction in the non-demyelinated normal appearing gray matter (NAGM) and prominently in the cerebellum. In contrast to early disease stages, where synaptic and neuro-axonal pathology correlates with the extent of T cell infiltration, a prominent role of the innate immune system has been proposed for progressive MS. However, the specific contribution of microglia and astrocytes to synaptic cerebellar pathology in the NAGM- independent of an adaptive T cell response - remains largely unexplored. In the present study, we quantified synaptic changes in the cerebellar NAGM distant from demyelinated lesions in a mouse model of toxic demyelination. Proteomic analysis of the cerebellar cortex revealed differential regulation of synaptic and glutamate transport proteins in the absence of evident structural synaptic pathology or local gray matter demyelination. At the functional level, synaptic changes manifested as a reduction in frequency-dependent facilitation at the parallel fiber- Purkinje cell synapse. Further, deficiency of MyD88, an adaptor protein of the innate immune response, associated with a functional recovery in facilitation, reduced changes in the differential expression of synaptic and glutamate transport proteins, and reduced transcription levels of inflammatory cytokines. Nevertheless, the characteristics of demyelinating lesions and their associated cellular response were similar to wild type animals. Our work brings forward an experimental paradigm mimicking the diffuse synaptic pathology independent of demyelination in late stage MS and highlights the complex regulation of synaptic pathology in the cerebellar NAGM. Moreover, our findings suggest a role of astrocytes, in particular Bergmann glia, as key cellular determinants of cerebellar synaptic dysfunction.

AB - Progressive neurological decline in multiple sclerosis is associated with axonal loss and synaptic dysfunction in the non-demyelinated normal appearing gray matter (NAGM) and prominently in the cerebellum. In contrast to early disease stages, where synaptic and neuro-axonal pathology correlates with the extent of T cell infiltration, a prominent role of the innate immune system has been proposed for progressive MS. However, the specific contribution of microglia and astrocytes to synaptic cerebellar pathology in the NAGM- independent of an adaptive T cell response - remains largely unexplored. In the present study, we quantified synaptic changes in the cerebellar NAGM distant from demyelinated lesions in a mouse model of toxic demyelination. Proteomic analysis of the cerebellar cortex revealed differential regulation of synaptic and glutamate transport proteins in the absence of evident structural synaptic pathology or local gray matter demyelination. At the functional level, synaptic changes manifested as a reduction in frequency-dependent facilitation at the parallel fiber- Purkinje cell synapse. Further, deficiency of MyD88, an adaptor protein of the innate immune response, associated with a functional recovery in facilitation, reduced changes in the differential expression of synaptic and glutamate transport proteins, and reduced transcription levels of inflammatory cytokines. Nevertheless, the characteristics of demyelinating lesions and their associated cellular response were similar to wild type animals. Our work brings forward an experimental paradigm mimicking the diffuse synaptic pathology independent of demyelination in late stage MS and highlights the complex regulation of synaptic pathology in the cerebellar NAGM. Moreover, our findings suggest a role of astrocytes, in particular Bergmann glia, as key cellular determinants of cerebellar synaptic dysfunction.

KW - Animals

KW - Mice

KW - Astrocytes/metabolism

KW - Signal Transduction/physiology

KW - Disease Models, Animal

KW - Synapses/metabolism

KW - Cerebellar Cortex/pathology

KW - Myeloid Differentiation Factor 88/metabolism

KW - Mice, Inbred C57BL

KW - Demyelinating Diseases/pathology

KW - Mice, Knockout

KW - Cuprizone/toxicity

KW - Male

UR - https://www.scopus.com/pages/publications/85218704784

U2 - 10.1186/s12974-025-03368-9

DO - 10.1186/s12974-025-03368-9

M3 - Article

C2 - 39988657

SN - 1742-2094

VL - 22

JO - Journal of Neuroinflammation

JF - Journal of Neuroinflammation

IS - 1

M1 - 47

ER -

Astroglial modulation of synaptic function in the non-demyelinated cerebellar cortex is dependent on MyD88 signaling in a model of toxic demyelination

Abstract

Austrian Fields of Science 2012

Keywords

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