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VAMP2/3 的裂解影响发育中鼠脊髓中的少突胶质前体细胞谱系发育。

Cleavage of VAMP2/3 Affects Oligodendrocyte Lineage Development in the Developing Mouse Spinal Cord.

机构信息

Department of Physiology and Neurobiology, University of Connecticut, Storrs, Connecticut 06269.

Department of Physiology and Neurobiology, University of Connecticut, Storrs, Connecticut 06269

出版信息

J Neurosci. 2023 Sep 27;43(39):6592-6608. doi: 10.1523/JNEUROSCI.2206-21.2023. Epub 2023 Aug 24.

Abstract

In the developing and adult CNS, new oligodendrocytes (OLs) are generated from a population of cells known as oligodendrocyte precursor cells (OPCs). As they begin to differentiate, OPCs undergo a series of highly regulated changes to morphology, gene expression, and membrane organization. This stage represents a critical bottleneck in oligodendrogliogenesis, and the regulatory program that guides it is still not fully understood. Here, we show that toxin-mediated cleavage of the vesicle associated SNARE proteins VAMP2/3 in the OL lineage of both male and female mice impairs the ability of early OLs to mature into functional, myelinating OLs. In the developing mouse spinal cord, many VAMP2/3-cleaved OLs appeared to stall in the premyelinating, early OL stage, resulting in an overall loss of both myelin density and OL number. The Src kinase Fyn, a key regulator of oligodendrogliogenesis and myelination, is highly expressed among premyelinating OLs, but its expression decreases as OLs mature. We found that OLs with cleaved VAMP2/3 in the spinal cord white matter showed significantly higher expression of Fyn compared with neighboring control cells, potentially because of an extended premyelinating stage. Overall, our results show that functional VAMP2/3 in OL lineage cells is essential for proper myelin formation and plays a major role in controlling the maturation and terminal differentiation of premyelinating OLs. The production of mature oligodendrocytes (OLs) is essential for CNS myelination during development, myelin remodeling in adulthood, and remyelination following injury or in demyelinating disease. Before myelin sheath formation, newly formed OLs undergo a series of highly regulated changes during a stage of their development known as the premyelinating, or early OL stage. This stage acts as a critical checkpoint in OL development, and much is still unknown about the dynamic regulatory processes involved. In this study, we show that VAMP2/3, SNARE proteins involved in vesicular trafficking and secretion play an essential role in regulating premyelinating OL development and are required for healthy myelination in the developing mouse spinal cord.

摘要

在中枢神经系统(CNS)的发育和成熟过程中,新的少突胶质细胞(OL)是由一类称为少突胶质前体细胞(OPC)的细胞产生的。当它们开始分化时,OPC 经历了一系列形态、基因表达和膜组织的高度调节变化。这个阶段代表了少突胶质细胞发生的一个关键瓶颈,而指导这一过程的调控程序仍不完全清楚。在这里,我们表明,毒素介导的囊泡相关 SNARE 蛋白 VAMP2/3 在雄性和雌性小鼠 OL 谱系中的切割,会损害早期 OL 成熟为功能性髓鞘形成 OL 的能力。在发育中的小鼠脊髓中,许多 VAMP2/3 被切割的 OL 似乎停滞在预髓鞘形成的早期 OL 阶段,导致髓鞘密度和 OL 数量的整体损失。Src 激酶 Fyn 是少突胶质细胞发生和髓鞘形成的关键调节因子,在预髓鞘形成的 OL 中高度表达,但随着 OL 的成熟,其表达减少。我们发现,脊髓白质中 VAMP2/3 被切割的 OL 与相邻的对照细胞相比,Fyn 的表达显著升高,这可能是由于预髓鞘形成阶段延长。总的来说,我们的结果表明,OL 谱系细胞中功能性 VAMP2/3 对于正常髓鞘形成是必不可少的,并且在控制预髓鞘形成 OL 的成熟和终末分化方面起着主要作用。成熟少突胶质细胞(OL)的产生对于中枢神经系统(CNS)在发育过程中的髓鞘形成、成年期的髓鞘重塑以及损伤或脱髓鞘疾病后的髓鞘再生是必不可少的。在形成髓鞘鞘之前,新形成的 OL 在它们的发育过程中的一个阶段经历了一系列高度调节的变化,这个阶段称为预髓鞘形成或早期 OL 阶段。这个阶段是 OL 发育的一个关键检查点,涉及的动态调节过程仍知之甚少。在这项研究中,我们表明,参与囊泡运输和分泌的 SNARE 蛋白 VAMP2/3 在调节预髓鞘形成 OL 的发育中起着至关重要的作用,并且是发育中的小鼠脊髓中健康髓鞘形成所必需的。

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