Department of Molecular Cell Biology, Weizmann Institute of Science, Rehovot, 76100, Israel.
Department of Life Sciences Core Facilities, Weizmann Institute of Science, Rehovot, 76100, Israel.
J Neurosci. 2020 Aug 5;40(32):6103-6111. doi: 10.1523/JNEUROSCI.0912-20.2020. Epub 2020 Jun 29.
Oligodendrocyte myelination depends on actin cytoskeleton rearrangement. Neural Wiskott-Aldrich syndrome protein(N-Wasp) is an actin nucleation factor that promotes polymerization of branched actin filaments. N-Wasp activity is essential for myelin membrane wrapping by Schwann cells, but its role in oligodendrocytes and CNS myelination remains unknown. Here we report that oligodendrocytes-specific deletion of in mice of both sexes resulted in hypomyelination (i.e., reduced number of myelinated axons and thinner myelin profiles), as well as substantial focal hypermyelination reflected by the formation of remarkably long myelin outfolds. These myelin outfolds surrounded unmyelinated axons, neuronal cell bodies, and other myelin profiles. The latter configuration resulted in pseudo-multimyelin profiles that were often associated with axonal detachment and degeneration throughout the CNS, including in the optic nerve, corpus callosum, and the spinal cord. Furthermore, developmental analysis revealed that myelin abnormalities were already observed during the onset of myelination, suggesting that they are formed by aberrant and misguided elongation of the oligodendrocyte inner lip membrane. Our results demonstrate that N-Wasp is required for the formation of normal myelin in the CNS. They also reveal that N-Wasp plays a distinct role in oligodendrocytes compared with Schwann cells, highlighting a difference in the regulation of actin dynamics during CNS and PNS myelination. Myelin is critical for the normal function of the nervous system by facilitating fast conduction of action potentials. During the process of myelination in the CNS, oligodendrocytes undergo extensive morphological changes that involve cellular process extension and retraction, axonal ensheathment, and myelin membrane wrapping. Here we present evidence that N-Wasp, a protein regulating actin filament assembly through Arp2/3 complex-dependent actin nucleation, plays a critical role in CNS myelination, and its absence leads to several myelin abnormalities. Our data provide an important step into the understanding of the molecular mechanisms underlying CNS myelination.
少突胶质细胞髓鞘形成依赖于肌动蛋白细胞骨架的重排。神经 Wiskott-Aldrich 综合征蛋白(N-WASP)是一种肌动蛋白成核因子,可促进分支肌动蛋白丝的聚合。N-WASP 的活性对施万细胞包裹髓鞘膜至关重要,但它在少突胶质细胞和中枢神经系统髓鞘形成中的作用尚不清楚。在这里,我们报告在雌雄小鼠中特异性敲除 导致少突胶质细胞少突胶质化(即,少突胶质细胞包裹的轴突数量减少和髓鞘厚度变薄),以及由非常长的髓鞘褶皱形成引起的显著局灶性过度髓鞘化。这些髓鞘褶皱围绕着未髓鞘化的轴突、神经元胞体和其他髓鞘。后一种结构导致假多核髓鞘,这些髓鞘常与整个中枢神经系统中的轴突脱离和变性有关,包括视神经、胼胝体和脊髓。此外,发育分析表明,髓鞘异常在髓鞘形成开始时就已经观察到,这表明它们是由少突胶质细胞内唇膜的异常和误导性伸长形成的。我们的结果表明,N-WASP 是中枢神经系统中正常髓鞘形成所必需的。它们还表明,N-WASP 在少突胶质细胞中的作用与施万细胞不同,突出了在中枢神经系统和周围神经系统髓鞘形成过程中肌动蛋白动力学调节的差异。髓鞘通过促进动作电位的快速传导对神经系统的正常功能至关重要。在中枢神经系统的髓鞘形成过程中,少突胶质细胞经历广泛的形态变化,包括细胞过程的延伸和回缩、轴突包绕和髓鞘膜包裹。在这里,我们提供的证据表明,N-WASP 是一种通过 Arp2/3 复合物依赖性肌动蛋白成核调节肌动蛋白丝组装的蛋白质,在中枢神经系统髓鞘形成中起关键作用,其缺失会导致多种髓鞘异常。我们的数据为理解中枢神经系统髓鞘形成的分子机制提供了重要的一步。
