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首页> 外文期刊>The Journal of biological chemistry >A Multi-domain Fragment of Nogo-A Protein Is a Potent Inhibitor of Cortical Axon Regeneration via Nogo Receptor 1
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A Multi-domain Fragment of Nogo-A Protein Is a Potent Inhibitor of Cortical Axon Regeneration via Nogo Receptor 1

机译:Nogo-A蛋白的多域片段是通过Nogo受体1的皮质轴突再生的有效抑制剂

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Nogo-A limits axon regeneration and functional recovery after central nervous system injury in adult mammals. Three regions of Nogo-A (Nogo-A-24, Nogo-66, and Nogo-C39) interact with the neuronal Nogo-66 receptor 1 (NgR1). Nogo-66 also interacts with a structurally unrelated cell surface receptor, paired immunoglobulin-like receptor (PirB). We show here that the other two NgR1-interacting domains, Nogo-A-24 and Nogo-C39, also bind to PirB with high affinity. A purified 22-kDa protein containing all three NgR1- and PirB-interacting domains (Nogo-22) is a substantially more potent growth cone-collapsing molecule than Nogo-66 for chick dorsal root ganglion neurons and mature cortical neurons. Moreover, Nogo-22 inhibits axon regeneration of mature cortical neurons in vitro more potently than does Nogo-66. Although all three NgR1-interacting domains of Nogo-A also interact with PirB, expression of PirB in mature cortical cultures is nearly undetectable. Consistent with a relatively minor role for PirB in mature cortical neurons, Nogo-22 inhibition of axon regeneration is abolished by genetic deletion of NgR1. Thus, NgR1 is the predominant receptor for Nogo-22 in regenerating cortical neurons.
机译:Nogo-a限制成年哺乳动物中枢神经系统损伤后的轴突再生和功能恢复。 Nogo-A(Nogo-A-24,Nogo-66和Nogo-C39)的三个区域与神经元Nogo-66受体1相互作用。 Nogo-66还与结构性无关的细胞表面受体,配对的免疫球蛋白样受体(PIRB)相互作用。我们在这里展示另外两个NGR1相互作用的结构域,Nogo-A-24和Nogo-C39,也与高亲和力的PIRB结合。含有所有三个NGR1和PIRB相互作用结构域(Nogo-22)的纯化的22-KDA蛋白质是比Nogo-66为小鸡背根神经节神经元和成熟皮质神经元的基本上更有效的生长锥塌陷的分子。此外,Nogo-22抑制了成熟皮质神经元的轴突再生,而不是Nogo-66更易于效果。尽管诺罗-A的所有三个嵌段相互作用的结构域也与PIRB相互作用,但成熟皮质培养物中的PIRB的表达几乎无法检测到。与成熟皮质神经元中的PIRB相对较小的作用一致,通过NGR1的遗传缺失废除了Nogo-22轴突再生的抑制。因此,NGR1是在再生皮质神经元中的Nogo-22的主要受体。

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