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首页> 外文期刊>Journal of Neurochemistry: Offical Journal of the International Society for Neurochemistry >Binding of soluble myelin-associated glycoprotein to specific gangliosides induces the association of p75 to lipid rafts and signal transduction.
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Binding of soluble myelin-associated glycoprotein to specific gangliosides induces the association of p75 to lipid rafts and signal transduction.

机译:可溶性髓鞘相关糖蛋白与特定神经节苷脂的结合诱导p75与脂质筏和信号转导的缔合。

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摘要

Abstract Myelin-associated glycoprotein (MAG) is a potent inhibitor of neurite outgrowth from a variety of neurons. Here we show that gangliosides, GT1b and GD1a, as well as the Nogo receptor, are functional binding partners for soluble MAG-Fc. Postnatal cerebellar neurons from mice deficient in the GalNAcT gene are insensitive to MAG with regard to neurite outgrowth and lack in the activation of RhoA. MAG-Fc or the antibody to GT1b and GD1a elicits recruitment of p75(NTR.) to lipid rafts, specialized microdomain for signal transduction. Disruption of lipid rafts results in abolishment of inhibitory effects of MAG-Fc and the Nogo peptide. These findings establish gangliosides as functional binding partners for soluble MAG. Gangliosides may play a role in translocation of p75(NTR.) to lipid rafts for initiation of the signal transduction.
机译:摘要髓鞘相关糖蛋白(MAG)是一种有效的神经突生长抑制作用,可抑制多种神经元的生长。在这里,我们显示神经节苷脂,GT1b和GD1a以及Nogo受体是可溶性MAG-Fc的功能性结合伴侣。来自GalNAcT基因缺陷的小鼠的产后小脑神经元对神经突生长和缺乏RhoA激活均对MAG不敏感。 MAG-Fc或针对GT1b和GD1a的抗体引发p75(NTR。)募集至脂质筏,该筏是信号转导的专门微区。脂质筏的破坏导致MAG-Fc和Nogo肽的抑制作用消失。这些发现建立了神经节苷脂作为可溶性MAG的功能性结合伴侣。神经节苷脂可能在将p75(NTR。)转运到脂质筏中以启动信号转导中发挥作用。

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