Localized microglia dysregulation impairs central nervous system myelination in development

Rebecca K Holloway; Liang  Zhang; Irene Molina-Gonzalez; Kathy Ton; James A R Nicoll; James P Boardman; Yan Liang; Anna C Williams; Véronique E Miron

doi:10.1186/s40478-023-01543-8

Localized microglia dysregulation impairs central nervous system myelination in development

Rebecca K Holloway, Liang Zhang, Irene Molina-Gonzalez, Kathy Ton, James A R Nicoll, James P Boardman, Yan Liang, Anna C Williams, Véronique E Miron^*

^*Corresponding author for this work

Research output: Contribution to journal › Article › peer-review

Abstract

Myelination of neuronal axons is a critical aspect of central nervous system development and function. However, the fundamental cellular and molecular mechanisms influencing human developmental myelination and its failure are not fully understood. Here, we used digital spatial transcriptomics of a rare bank of human developing white matter to uncover that a localized dysregulated innate immune response is associated with impeded myelination. We identified that poorly myelinating areas have a distinct signature of Type II interferon signalling in microglia/macrophages, relative to adjacent myelinating areas. This is associated with a surprising increase in mature oligodendrocytes, which fail to form myelin processes appropriately. We functionally link these findings by showing that conditioned media from interferon-stimulated microglia is sufficient to dysregulate myelin process formation by oligodendrocytes in culture. We identify the Type II interferon inducer, Osteopontin (SPP1), as being upregulated in poorly myelinating brains, indicating a potential biomarker. Our results reveal the importance of microglia-mature oligodendrocyte interaction and interferon signaling in regulating myelination of the developing human brain.

Original language	English
Article number	49
Number of pages	15
Journal	Acta Neuropathologica Communications
Volume	11
DOIs	https://doi.org/10.1186/s40478-023-01543-8
Publication status	Published - 23 Mar 2023

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title = "Localized microglia dysregulation impairs central nervous system myelination in development",

abstract = "Myelination of neuronal axons is a critical aspect of central nervous system development and function. However, the fundamental cellular and molecular mechanisms influencing human developmental myelination and its failure are not fully understood. Here, we used digital spatial transcriptomics of a rare bank of human developing white matter to uncover that a localized dysregulated innate immune response is associated with impeded myelination. We identified that poorly myelinating areas have a distinct signature of Type II interferon signalling in microglia/macrophages, relative to adjacent myelinating areas. This is associated with a surprising increase in mature oligodendrocytes, which fail to form myelin processes appropriately. We functionally link these findings by showing that conditioned media from interferon-stimulated microglia is sufficient to dysregulate myelin process formation by oligodendrocytes in culture. We identify the Type II interferon inducer, Osteopontin (SPP1), as being upregulated in poorly myelinating brains, indicating a potential biomarker. Our results reveal the importance of microglia-mature oligodendrocyte interaction and interferon signaling in regulating myelination of the developing human brain.",

author = "Holloway, \{Rebecca K\} and Liang Zhang and Irene Molina-Gonzalez and Kathy Ton and Nicoll, \{James A R\} and Boardman, \{James P\} and Yan Liang and Williams, \{Anna C\} and Miron, \{V{\'e}ronique E\}",

note = "Funding Information: This study was funded by a Nanostring Technologies, Inc. Human Cell Atlas Grant (A.W. and V.E.M.), Medical Research Council Senior Non-Clinical Fellowship (MR/V031260/1, V.E.M.), The Anne Rowling Regenerative Neurology Clinic (V.E.M.), Save Our Babies (V.E.M.), Medical Research Council Centre for Reproductive Health (MR/N02256/1), Theirworld (J.P.B), and the John David Eaton Chair in Multiple Sclerosis Research (V.E.M.). Publisher Copyright: {\textcopyright} 2023, The Author(s).",

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AU - Holloway, Rebecca K

AU - Zhang, Liang

AU - Molina-Gonzalez, Irene

AU - Ton, Kathy

AU - Nicoll, James A R

AU - Boardman, James P

AU - Liang, Yan

AU - Williams, Anna C

AU - Miron, Véronique E

N1 - Funding Information: This study was funded by a Nanostring Technologies, Inc. Human Cell Atlas Grant (A.W. and V.E.M.), Medical Research Council Senior Non-Clinical Fellowship (MR/V031260/1, V.E.M.), The Anne Rowling Regenerative Neurology Clinic (V.E.M.), Save Our Babies (V.E.M.), Medical Research Council Centre for Reproductive Health (MR/N02256/1), Theirworld (J.P.B), and the John David Eaton Chair in Multiple Sclerosis Research (V.E.M.). Publisher Copyright: © 2023, The Author(s).

PY - 2023/3/23

Y1 - 2023/3/23

N2 - Myelination of neuronal axons is a critical aspect of central nervous system development and function. However, the fundamental cellular and molecular mechanisms influencing human developmental myelination and its failure are not fully understood. Here, we used digital spatial transcriptomics of a rare bank of human developing white matter to uncover that a localized dysregulated innate immune response is associated with impeded myelination. We identified that poorly myelinating areas have a distinct signature of Type II interferon signalling in microglia/macrophages, relative to adjacent myelinating areas. This is associated with a surprising increase in mature oligodendrocytes, which fail to form myelin processes appropriately. We functionally link these findings by showing that conditioned media from interferon-stimulated microglia is sufficient to dysregulate myelin process formation by oligodendrocytes in culture. We identify the Type II interferon inducer, Osteopontin (SPP1), as being upregulated in poorly myelinating brains, indicating a potential biomarker. Our results reveal the importance of microglia-mature oligodendrocyte interaction and interferon signaling in regulating myelination of the developing human brain.

AB - Myelination of neuronal axons is a critical aspect of central nervous system development and function. However, the fundamental cellular and molecular mechanisms influencing human developmental myelination and its failure are not fully understood. Here, we used digital spatial transcriptomics of a rare bank of human developing white matter to uncover that a localized dysregulated innate immune response is associated with impeded myelination. We identified that poorly myelinating areas have a distinct signature of Type II interferon signalling in microglia/macrophages, relative to adjacent myelinating areas. This is associated with a surprising increase in mature oligodendrocytes, which fail to form myelin processes appropriately. We functionally link these findings by showing that conditioned media from interferon-stimulated microglia is sufficient to dysregulate myelin process formation by oligodendrocytes in culture. We identify the Type II interferon inducer, Osteopontin (SPP1), as being upregulated in poorly myelinating brains, indicating a potential biomarker. Our results reveal the importance of microglia-mature oligodendrocyte interaction and interferon signaling in regulating myelination of the developing human brain.

U2 - 10.1186/s40478-023-01543-8

DO - 10.1186/s40478-023-01543-8

M3 - Article

SN - 2051-5960

VL - 11

JO - Acta Neuropathologica Communications

JF - Acta Neuropathologica Communications

M1 - 49

ER -

Localized microglia dysregulation impairs central nervous system myelination in development

Abstract

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