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Wnt5a 与 Wnt-平面细胞极性通路协同促进轴突伸长。

Wnt5a Promotes Axon Elongation in Coordination with the Wnt-Planar Cell Polarity Pathway.

机构信息

Department of Biochemistry, Donnelly Centre, University of Toronto, Toronto, ON M5S 3E1, Canada.

出版信息

Cells. 2024 Jul 28;13(15):1268. doi: 10.3390/cells13151268.

Abstract

The establishment of neuronal polarity, involving axon specification and outgrowth, is critical to achieve the proper morphology of neurons, which is important for neuronal connectivity and cognitive functions. Extracellular factors, such as Wnts, modulate diverse aspects of neuronal morphology. In particular, non-canonical Wnt5a exhibits differential effects on neurite outgrowth depending upon the context. Thus, the role of Wnt5a in axon outgrowth and neuronal polarization is not completely understood. In this study, we demonstrate that Wnt5a, but not Wnt3a, promotes axon outgrowth in dissociated mouse embryonic cortical neurons and does so in coordination with the core PCP components, Prickle and Vangl. Unexpectedly, exogenous Wnt5a-induced axon outgrowth was dependent on endogenous, neuronal Wnts, as the chemical inhibition of Porcupine using the IWP2- and siRNA-mediated knockdown of either Porcupine or Wntless inhibited Wnt5a-induced elongation. Importantly, delayed treatment with IWP2 did not block Wnt5a-induced elongation, suggesting that endogenous Wnts and Wnt5a act during specific timeframes of neuronal polarization. Wnt5a in fibroblast-conditioned media can associate with small extracellular vesicles (sEVs), and we also show that these Wnt5a-containing sEVs are primarily responsible for inducing axon elongation.

摘要

神经元极性的建立,涉及轴突的特化和生长,对于神经元的适当形态至关重要,这对于神经元的连接和认知功能很重要。细胞外因子,如 Wnts,调节神经元形态的多个方面。特别是非经典的 Wnt5a 根据上下文对神经突生长表现出不同的影响。因此,Wnt5a 在轴突生长和神经元极化中的作用尚不完全清楚。在这项研究中,我们证明了 Wnt5a(而非 Wnt3a)促进了分离的小鼠胚胎皮质神经元的轴突生长,并且这种作用与核心 PCP 成分 Prickle 和 Vangl 协调。出乎意料的是,外源性 Wnt5a 诱导的轴突生长依赖于内源性神经元 Wnts,因为使用化学抑制剂 IWP2 和针对 Porcupine 的 siRNA 敲低 Porcupine 或 Wntless 抑制了 Wnt5a 诱导的伸长。重要的是,延迟用 IWP2 处理不会阻断 Wnt5a 诱导的伸长,这表明内源性 Wnts 和 Wnt5a 在神经元极化的特定时间框架内发挥作用。成纤维细胞条件培养基中的 Wnt5a 可以与小细胞外囊泡 (sEVs) 结合,我们还表明,这些含有 Wnt5a 的 sEVs 主要负责诱导轴突伸长。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e5ba/11312420/11779040bdc5/cells-13-01268-g001.jpg

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