首页> 外文期刊>The Journal of Neuroscience: The Official Journal of the Society for Neuroscience >Neurotrophin-3 sorts to the constitutive secretory pathway of hippocampal neurons and is diverted to the regulated secretory pathway by coexpression with brain-derived neurotrophic factor.
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Neurotrophin-3 sorts to the constitutive secretory pathway of hippocampal neurons and is diverted to the regulated secretory pathway by coexpression with brain-derived neurotrophic factor.

机译:Neurotrophin-3排序到海马神经元的组成型分泌途径,并通过与脑源性神经营养因子的共表达转移到调节的分泌途径。

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摘要

Hippocampal neurons release nerve growth factor (NGF) through the constitutive secretory pathway, thus allowing the protein to be continuously available for promoting nerve cell survival. In contrast, hippocampal neurons use the regulated secretory pathway to process brain-derived neurotrophic factor (BDNF), which alters synaptic activity when released acutely from dense-core vesicles. Thus, understanding how neurons sort and deliver neurotrophins may provide clues to their functions in brain. In this study, we monitored the processing and delivery of neurotrophin-3 (NT-3). Pulse-chase studies, immunocytochemistry, and secretagogue-induced release experiments were performed on cultured hippocampal neurons and AtT-20 cells infected with vaccinia viruses encoding the NT-3 precursor (pro-NT-3). Results show that most newly synthesized NT-3 is released through the constitutive secretory pathway as a result of furin-mediated endoproteolytic cleavage of pro-NT-3 in the trans-Golgi network. Pro-NT-3 can also be diverted into the regulated secretory pathway when cells are treated with alpha1-PDX, a selective inhibitor of furin-like enzymes, or when pro-NT-3 expression is increased by transient transfection methods. In cells coinfected with viruses coding for pro-NT-3 and pro-BDNF, NT-3 is sorted into the regulated pathway, stored in secretory granules, and released in response to extracellular cues together with BDNF, apparently as a result of heterodimerization, as suggested by coimmunoprecipitation data. Taken together, these data show that sorting of the NT-3 precursor can occur in both the constitutive and regulated secretory pathways, which is consistent with NT-3 having both survival-promoting and synapse-altering functions.
机译:海马神经元通过组成型分泌途径释放神经生长因子(NGF),从而使该蛋白可连续用于促进神经细胞存活。相比之下,海马神经元使用调节的分泌途径来处理脑源性神经营养因子(BDNF),当从密集核心囊泡急性释放时,它会改变突触活性。因此,了解神经元如何分类和传递神经营养蛋白可能为它们在大脑中的功能提供线索。在这项研究中,我们监测了神经营养蛋白3(NT-3)的加工和传递。在培养的海马神经元和被编码NT-3前体(pro-NT-3)的牛痘病毒感染的AtT-20细胞上进行了脉冲追踪研究,免疫细胞化学和促分泌素诱导的释放实验。结果表明,由于弗林蛋白酶介导的反式高尔基体网络中pro-NT-3的内蛋白水解裂解,大多数新合成的NT-3通过组成型分泌途径释放。当用α1-PDX(一种弗林蛋白酶样酶的选择性抑制剂)处理细胞,或通过瞬时转染方法增加pro-NT-3的表达时,Pro-NT-3也可以转移到调节的分泌途径中。在感染了编码pro-NT-3和pro-BDNF的病毒的细胞中,NT-3被归类为受调节的途径,存储在分泌颗粒中,并响应于BDNF一起与胞外信号一起释放,这显然是异源二聚化的结果,根据免疫共沉淀数据的建议。总而言之,这些数据表明NT-3前体的分选可以在组成型和调节型分泌途径中发生,这与具有生存促进功能和突触改变功能的NT-3一致。

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