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

IF 5.4 2区 医学 Q1 NEUROSCIENCES
Glia Pub Date : 2024-07-18 DOI:10.1002/glia.24589
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
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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.

Abstract Image

髓鞘碱性蛋白 mRNA 水平会影响髓鞘的尺寸、结构、可塑性和常驻神经胶质细胞的密度。
髓鞘碱性蛋白(Mbp)对中枢神经系统髓鞘的形成和维持至关重要,其积累减少会导致髓鞘化不足。不同的 Mbp mRNA 水平如何影响整个生命周期的髓鞘尺寸,以及驻留神经胶质细胞如何应对这种变化,这些都是未知的。为了研究这些问题,我们使用了增强子编辑的小鼠品系,这些品系积累的 Mbp mRNA 水平是野生型的 8% 到 160%。在幼鼠中,Mbp mRNA水平的降低导致了Mbp蛋白积累和髓鞘厚度的相应减少,这证实了之前证实的Mbp转录在控制初始髓鞘合成中的限速作用。然而,尽管到老年期Mbp mRNA水平仍较低,但Mbp蛋白水平和髓鞘厚度都有所改善或完全正常化,其速度取决于Mbp mRNA的相对水平。相反,只有当 mRNA 水平很低时,鞘的长度才会受到影响,这表明鞘的厚度和长度与 Mbp mRNA 水平的关系并不一样。随着 mRNA 水平的降低,鞘的结构也出现了明显的异常。令人意想不到的是,所有神经胶质细胞类型的密度都随着 Mbp mRNA 水平的降低而增加。这项研究拓展了人们对 Mbp 在小鼠整个生命周期的髓鞘形成、结构和可塑性中所扮演角色的认识,并揭示了神经胶质细胞串联的新轴心。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Glia
Glia 医学-神经科学
CiteScore
13.10
自引率
4.80%
发文量
162
审稿时长
3-8 weeks
期刊介绍: GLIA is a peer-reviewed journal, which publishes articles dealing with all aspects of glial structure and function. This includes all aspects of glial cell biology in health and disease.
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