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

髓鞘碱性蛋白 生物 髓鞘 信使核糖核酸 细胞生物学 蛋白脂蛋白1 少突胶质细胞 神经胶质 神经科学 中枢神经系统 生物化学 基因
作者
Hooman Bagheri,Hana Friedman,Amanda Hadwen,Celia Jarweh,Ellis Cooper,Lawrence Oprea,Claire Guerrier,Anmar Khadra,A. Collin,Julien Cohen‐Adad,Amanda Young,Gerardo Mendez Victoriano,Matthew Swire,Andrew A. Jarjour,Marie E. Bechler,Rachel S. Pryce,Pierre Chaurand,Lise Cougnaud,Dajana Vuckovic,Elliott M Wilion
出处
期刊:Glia [Wiley]
卷期号:72 (10): 1893-1914 被引量:4
标识
DOI:10.1002/glia.24589
摘要

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.
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