Thinning of originally-existing, mature myelin represents a nondestructive form of myelin loss in the adult CNS

Min Li Lin; Wensheng Lin

doi:10.3389/fncel.2025.1565913

Thinning of originally-existing, mature myelin represents a nondestructive form of myelin loss in the adult CNS

Min Li Lin, Wensheng Lin

Neuroscience

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

Abstract

The main function of oligodendrocytes is to assemble and maintain myelin that wraps and insulates axons in the central nervous system (CNS). Traditionally, myelin structure, particularly its thickness, was believed to remain remarkably stable in adulthood (including early and middle adulthood, but not late adulthood or aging). However, emerging evidence reveals that the thickness of originally-existing, mature myelin (OEM) can undergo dynamic changes in the adult CNS. This overview highlights recent findings on the alteration of OEM thickness in the adult CNS, explores the underlying mechanisms, and proposes that progressive thinning of OEM represents a novel, nondestructive form of myelin loss in myelin disorders of the CNS.

Original language	English (US)
Article number	1565913
Journal	Frontiers in Cellular Neuroscience
Volume	19
DOIs	https://doi.org/10.3389/fncel.2025.1565913
State	Published - 2025

Bibliographical note

Publisher Copyright:
Copyright © 2025 Lin and Lin.

Keywords

PERK
myelin
myelin disorder
myelin loss
myelin thickness
myelin thinning
oligodendrocyte

PubMed: MeSH publication types

Journal Article

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10.3389/fncel.2025.1565913

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abstract = "The main function of oligodendrocytes is to assemble and maintain myelin that wraps and insulates axons in the central nervous system (CNS). Traditionally, myelin structure, particularly its thickness, was believed to remain remarkably stable in adulthood (including early and middle adulthood, but not late adulthood or aging). However, emerging evidence reveals that the thickness of originally-existing, mature myelin (OEM) can undergo dynamic changes in the adult CNS. This overview highlights recent findings on the alteration of OEM thickness in the adult CNS, explores the underlying mechanisms, and proposes that progressive thinning of OEM represents a novel, nondestructive form of myelin loss in myelin disorders of the CNS.",

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author = "Lin, {Min Li} and Wensheng Lin",

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AU - Lin, Min Li

AU - Lin, Wensheng

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N2 - The main function of oligodendrocytes is to assemble and maintain myelin that wraps and insulates axons in the central nervous system (CNS). Traditionally, myelin structure, particularly its thickness, was believed to remain remarkably stable in adulthood (including early and middle adulthood, but not late adulthood or aging). However, emerging evidence reveals that the thickness of originally-existing, mature myelin (OEM) can undergo dynamic changes in the adult CNS. This overview highlights recent findings on the alteration of OEM thickness in the adult CNS, explores the underlying mechanisms, and proposes that progressive thinning of OEM represents a novel, nondestructive form of myelin loss in myelin disorders of the CNS.

AB - The main function of oligodendrocytes is to assemble and maintain myelin that wraps and insulates axons in the central nervous system (CNS). Traditionally, myelin structure, particularly its thickness, was believed to remain remarkably stable in adulthood (including early and middle adulthood, but not late adulthood or aging). However, emerging evidence reveals that the thickness of originally-existing, mature myelin (OEM) can undergo dynamic changes in the adult CNS. This overview highlights recent findings on the alteration of OEM thickness in the adult CNS, explores the underlying mechanisms, and proposes that progressive thinning of OEM represents a novel, nondestructive form of myelin loss in myelin disorders of the CNS.

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KW - myelin disorder

KW - myelin loss

KW - myelin thickness

KW - myelin thinning

KW - oligodendrocyte

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Thinning of originally-existing, mature myelin represents a nondestructive form of myelin loss in the adult CNS

Abstract

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Keywords

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