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Peripheral nerve axons contain machinery for co-translational secretion of axonally-generated proteins

机译:周围神经轴突包含轴突生成的蛋白质的共翻译分泌机制

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摘要

The axonal compartment of developing neurons and mature peripheral nervous system (PNS) neurons has the capacity to locally synthesize proteins. Axonally-synthesized proteins have been shown to facilitate axonal pathfinding and maintenance in developing central nervous system (CNS) and PNS neurons, and to facilitate the regeneration of mature PNS neurons. RNA-profiling studies of the axons of cultured neurons have shown a surprisingly complex population of mRNAs that encode proteins for a myriad of functions. Although classic-appearing rough endoplasmic reticulum (RER), smooth endoplasmic reticulum (ER) and Golgi apparatus have not been documented in axons by ultrastructural studies, axonal RNA profiling studies show several membrane and secreted protein-encoding mRNAs whose translation products would need access to a localized secretory mechanism. We previously showed that the axons of cultured neurons contain functional equivalents of RER and Golgi apparatus. Here, we show that markers for the signal-recognition particle, RER, ER, and Golgi apparatus are present in PNS axons in vivo. Co-localization of these proteins mirrors that seen for cultured axons where locally-translated proteins are localized to the axoplasmic membrane. Moreover, nerve injury increases the levels and/or aggregation of these proteins, suggesting that the regenerating axon has an increased capacity for membrane targeting of locally synthesized proteins.
机译:发育中的神经元和成熟的外周神经系统(PNS)神经元的轴突区室具有局部合成蛋白质的能力。轴突合成的蛋白质已显示出有助于发展中枢神经系统(CNS)和PNS神经元的轴突寻路和维持,并促进成熟PNS神经元的再生。对培养的神经元轴突的RNA谱研究表明,令人惊讶的复杂的mRNA种群能够编码具有多种功能的蛋白质。尽管超结构研究尚未在轴突中记录经典外观的粗面内质网(RER),平滑内质网(ER)和高尔基体,但轴突RNA谱研究显示了一些膜和分泌的蛋白质编码mRNA,其翻译产物需要通过局部的分泌机制。我们以前表明培养的神经元轴突包含RER和高尔基体的功能等效。在这里,我们显示信号识别粒子,RER,ER和高尔基体的标记存在于体内PNS轴突。这些蛋白质的共定位反映了在培养的轴突中看到的情况,其中局部翻译的蛋白质定位在轴质膜上。而且,神经损伤增加了这些蛋白质的水平和/或聚集,表明再生轴突具有提高的针对局部合成蛋白质的膜靶向的能力。

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