Myelin basic protein mRNA levels affect myelin sheath dimensions, architecture, plasticity, and density of resident glial cells

Hooman Bagheri; Hana Friedman; Amanda Hadwen; Celia Jarweh; Ellis Cooper; Lawrence Oprea; Claire Guerrier; Anmar Khadra; Armand Collin; Julien Cohen-Adad; Amanda Young; Gerardo Mendez Victoriano; Matthew Swire; Andrew Jarjour; Marie E. Bechler; Rachel S. Pryce; Pierre Chaurand; Lise Cougnaud; Dajana Vuckovic; Elliott Wilion; Owen Greene; Akiko Nishiyama; Anouk Benmamar-Badel; Trevor Owens; Vladimir Grouza; Marius Tuznik; Hanwen Liu; David A. Rudko; Jinyi Zhang; Katherine A. Siminovitch; Alan C. Peterson

doi:10.1002/glia.24589

Myelin basic protein mRNA levels affect myelin sheath dimensions, architecture, plasticity, and density of resident glial cells

Hooman Bagheri
, Hana Friedman
, Amanda Hadwen
, Celia Jarweh
, Ellis Cooper
, Lawrence Oprea
, Claire Guerrier
, Anmar Khadra
, Armand Collin
, Julien Cohen-Adad
, Amanda Young
, Gerardo Mendez Victoriano
, Matthew Swire
, Andrew Jarjour
, Marie E. Bechler
, Rachel S. Pryce
, Pierre Chaurand
, Lise Cougnaud
, Dajana Vuckovic
, Elliott Wilion

Owen Greene, Akiko Nishiyama, Anouk Benmamar-Badel, Trevor Owens, Vladimir Grouza, Marius Tuznik, Hanwen Liu, David A. Rudko, Jinyi Zhang, Katherine A. Siminovitch, Alan C. Peterson^*

^*Kontaktforfatter

Publikation: Bidrag til tidsskrift › Tidsskriftartikel › Forskning › peer review

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Abstract

Myelin basic protein (Mbp) is essential for both elaboration and maintenance of CNS myelin, and its reduced accumulation results in hypomyelination. How different Mbp mRNA levels affect myelin dimensions across the lifespan and how resident glial cells may respond to such changes are unknown. Here, to investigate these questions, we used enhancer-edited mouse lines that accumulate Mbp mRNA levels ranging from 8% to 160% of wild type. In young mice, reduced Mbp mRNA levels resulted in corresponding decreases in Mbp protein accumulation and myelin sheath thickness, confirming the previously demonstrated rate-limiting role of Mbp transcription in the control of initial myelin synthesis. However, despite maintaining lower line specific Mbp mRNA levels into old age, both Mbp protein levels and myelin thickness improved or fully normalized at rates defined by the relative Mbp mRNA level. Sheath length, in contrast, was affected only when mRNA levels were very low, demonstrating that sheath thickness and length are not equally coupled to Mbp mRNA level. Striking abnormalities in sheath structure also emerged with reduced mRNA levels. Unexpectedly, an increase in the density of all glial cell types arose in response to reduced Mbp mRNA levels. This investigation extends understanding of the role Mbp plays in myelin sheath elaboration, architecture, and plasticity across the mouse lifespan and illuminates a novel axis of glial cell crosstalk.

Originalsprog	Engelsk
Tidsskrift	Glia
Vol/bind	72
Udgave nummer	10
Sider (fra-til)	1893-1914
ISSN	0894-1491
DOI	https://doi.org/10.1002/glia.24589
Status	Udgivet - okt. 2024

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10.1002/glia.24589Licens: CC BY

Open Access VersionForlagets udgivne version, 9,04 MBLicens: CC BY

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Citationsformater

Bagheri, H., Friedman, H., Hadwen, A., Jarweh, C., Cooper, E., Oprea, L., Guerrier, C., Khadra, A., Collin, A., Cohen-Adad, J., Young, A., Victoriano, G. M., Swire, M., Jarjour, A., Bechler, M. E., Pryce, R. S., Chaurand, P., Cougnaud, L., Vuckovic, D., ... Peterson, A. C. (2024). Myelin basic protein mRNA levels affect myelin sheath dimensions, architecture, plasticity, and density of resident glial cells. Glia, 72(10), 1893-1914. https://doi.org/10.1002/glia.24589

@article{d06f9b82ba7c4ddead0874048a91e0f8,

title = "Myelin basic protein mRNA levels affect myelin sheath dimensions, architecture, plasticity, and density of resident glial cells",

abstract = "Myelin basic protein (Mbp) is essential for both elaboration and maintenance of CNS myelin, and its reduced accumulation results in hypomyelination. How different Mbp mRNA levels affect myelin dimensions across the lifespan and how resident glial cells may respond to such changes are unknown. Here, to investigate these questions, we used enhancer-edited mouse lines that accumulate Mbp mRNA levels ranging from 8\% to 160\% of wild type. In young mice, reduced Mbp mRNA levels resulted in corresponding decreases in Mbp protein accumulation and myelin sheath thickness, confirming the previously demonstrated rate-limiting role of Mbp transcription in the control of initial myelin synthesis. However, despite maintaining lower line specific Mbp mRNA levels into old age, both Mbp protein levels and myelin thickness improved or fully normalized at rates defined by the relative Mbp mRNA level. Sheath length, in contrast, was affected only when mRNA levels were very low, demonstrating that sheath thickness and length are not equally coupled to Mbp mRNA level. Striking abnormalities in sheath structure also emerged with reduced mRNA levels. Unexpectedly, an increase in the density of all glial cell types arose in response to reduced Mbp mRNA levels. This investigation extends understanding of the role Mbp plays in myelin sheath elaboration, architecture, and plasticity across the mouse lifespan and illuminates a novel axis of glial cell crosstalk.",

keywords = "astrocyte, hypermyelination, hypomyelination, Mbp transcription, microglia, myelin basic protein, myelin elaboration and plasticity, myelin sheath thickness and length, oligodendrocyte and oligodendrocyte progenitor cell, Myelin Basic Protein/metabolism, Mice, Inbred C57BL, Mice, Transgenic, Male, RNA, Messenger/metabolism, Neuroglia/metabolism, Animals, Mice, Myelin Sheath/metabolism",

author = "Hooman Bagheri and Hana Friedman and Amanda Hadwen and Celia Jarweh and Ellis Cooper and Lawrence Oprea and Claire Guerrier and Anmar Khadra and Armand Collin and Julien Cohen-Adad and Amanda Young and Victoriano, \{Gerardo Mendez\} and Matthew Swire and Andrew Jarjour and Bechler, \{Marie E.\} and Pryce, \{Rachel S.\} and Pierre Chaurand and Lise Cougnaud and Dajana Vuckovic and Elliott Wilion and Owen Greene and Akiko Nishiyama and Anouk Benmamar-Badel and Trevor Owens and Vladimir Grouza and Marius Tuznik and Hanwen Liu and Rudko, \{David A.\} and Jinyi Zhang and Siminovitch, \{Katherine A.\} and Peterson, \{Alan C.\}",

year = "2024",

month = oct,

doi = "10.1002/glia.24589",

language = "English",

volume = "72",

pages = "1893--1914",

journal = "Glia",

issn = "0894-1491",

publisher = "Wiley",

number = "10",

}

Bagheri, H, Friedman, H, Hadwen, A, Jarweh, C, Cooper, E, Oprea, L, Guerrier, C, Khadra, A, Collin, A, Cohen-Adad, J, Young, A, Victoriano, GM, Swire, M, Jarjour, A, Bechler, ME, Pryce, RS, Chaurand, P, Cougnaud, L, Vuckovic, D, Wilion, E, Greene, O, Nishiyama, A, Benmamar-Badel, A, Owens, T, Grouza, V, Tuznik, M, Liu, H, Rudko, DA, Zhang, J, Siminovitch, KA & Peterson, AC 2024, 'Myelin basic protein mRNA levels affect myelin sheath dimensions, architecture, plasticity, and density of resident glial cells', Glia, bind 72, nr. 10, s. 1893-1914. https://doi.org/10.1002/glia.24589

TY - JOUR

T1 - Myelin basic protein mRNA levels affect myelin sheath dimensions, architecture, plasticity, and density of resident glial cells

AU - Bagheri, Hooman

AU - Friedman, Hana

AU - Hadwen, Amanda

AU - Jarweh, Celia

AU - Cooper, Ellis

AU - Oprea, Lawrence

AU - Guerrier, Claire

AU - Khadra, Anmar

AU - Collin, Armand

AU - Cohen-Adad, Julien

AU - Young, Amanda

AU - Victoriano, Gerardo Mendez

AU - Swire, Matthew

AU - Jarjour, Andrew

AU - Bechler, Marie E.

AU - Pryce, Rachel S.

AU - Chaurand, Pierre

AU - Cougnaud, Lise

AU - Vuckovic, Dajana

AU - Wilion, Elliott

AU - Greene, Owen

AU - Nishiyama, Akiko

AU - Benmamar-Badel, Anouk

AU - Owens, Trevor

AU - Grouza, Vladimir

AU - Tuznik, Marius

AU - Liu, Hanwen

AU - Rudko, David A.

AU - Zhang, Jinyi

AU - Siminovitch, Katherine A.

AU - Peterson, Alan C.

PY - 2024/10

Y1 - 2024/10

N2 - Myelin basic protein (Mbp) is essential for both elaboration and maintenance of CNS myelin, and its reduced accumulation results in hypomyelination. How different Mbp mRNA levels affect myelin dimensions across the lifespan and how resident glial cells may respond to such changes are unknown. Here, to investigate these questions, we used enhancer-edited mouse lines that accumulate Mbp mRNA levels ranging from 8% to 160% of wild type. In young mice, reduced Mbp mRNA levels resulted in corresponding decreases in Mbp protein accumulation and myelin sheath thickness, confirming the previously demonstrated rate-limiting role of Mbp transcription in the control of initial myelin synthesis. However, despite maintaining lower line specific Mbp mRNA levels into old age, both Mbp protein levels and myelin thickness improved or fully normalized at rates defined by the relative Mbp mRNA level. Sheath length, in contrast, was affected only when mRNA levels were very low, demonstrating that sheath thickness and length are not equally coupled to Mbp mRNA level. Striking abnormalities in sheath structure also emerged with reduced mRNA levels. Unexpectedly, an increase in the density of all glial cell types arose in response to reduced Mbp mRNA levels. This investigation extends understanding of the role Mbp plays in myelin sheath elaboration, architecture, and plasticity across the mouse lifespan and illuminates a novel axis of glial cell crosstalk.

AB - Myelin basic protein (Mbp) is essential for both elaboration and maintenance of CNS myelin, and its reduced accumulation results in hypomyelination. How different Mbp mRNA levels affect myelin dimensions across the lifespan and how resident glial cells may respond to such changes are unknown. Here, to investigate these questions, we used enhancer-edited mouse lines that accumulate Mbp mRNA levels ranging from 8% to 160% of wild type. In young mice, reduced Mbp mRNA levels resulted in corresponding decreases in Mbp protein accumulation and myelin sheath thickness, confirming the previously demonstrated rate-limiting role of Mbp transcription in the control of initial myelin synthesis. However, despite maintaining lower line specific Mbp mRNA levels into old age, both Mbp protein levels and myelin thickness improved or fully normalized at rates defined by the relative Mbp mRNA level. Sheath length, in contrast, was affected only when mRNA levels were very low, demonstrating that sheath thickness and length are not equally coupled to Mbp mRNA level. Striking abnormalities in sheath structure also emerged with reduced mRNA levels. Unexpectedly, an increase in the density of all glial cell types arose in response to reduced Mbp mRNA levels. This investigation extends understanding of the role Mbp plays in myelin sheath elaboration, architecture, and plasticity across the mouse lifespan and illuminates a novel axis of glial cell crosstalk.

KW - astrocyte

KW - hypermyelination

KW - hypomyelination

KW - Mbp transcription

KW - microglia

KW - myelin basic protein

KW - myelin elaboration and plasticity

KW - myelin sheath thickness and length

KW - oligodendrocyte and oligodendrocyte progenitor cell

KW - Myelin Basic Protein/metabolism

KW - Mice, Inbred C57BL

KW - Mice, Transgenic

KW - Male

KW - RNA, Messenger/metabolism

KW - Neuroglia/metabolism

KW - Animals

KW - Mice

KW - Myelin Sheath/metabolism

U2 - 10.1002/glia.24589

DO - 10.1002/glia.24589

M3 - Journal article

C2 - 39023138

AN - SCOPUS:85198709822

SN - 0894-1491

VL - 72

SP - 1893

EP - 1914

JO - Glia

JF - Glia

IS - 10

ER -

Myelin basic protein mRNA levels affect myelin sheath dimensions, architecture, plasticity, and density of resident glial cells

Abstract

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