首页> 外文期刊>Genes and Development: a Journal Devoted to the Molecular Analysis of Gene Expression in Eukaryotes, Prokaryotes, and Viruses >The microtubule regulator ringer functions downstream from the RNA repair/splicing pathway to promote axon regeneration
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The microtubule regulator ringer functions downstream from the RNA repair/splicing pathway to promote axon regeneration

机译:微管稳压器铃声从RNA修复/拼接路线下游功能,以促进轴突再生

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摘要

Promoting axon regeneration in the central and peripheral nervous system is of clinical importance in neural injury and neurodegenerative diseases. Both pro- and antiregeneration factors are being identified. We previously reported that the Rtca mediated RNA repair/splicing pathway restricts axon regeneration by inhibiting the nonconventional splicing of Xbp1 mRNA under cellular stress. However, the downstream effectors remain unknown. Here, through transcriptome profiling, we show that the tubulin polymerization-promoting protein (TPPP) ringmaker/ringer is dramatically increased in Rtca-deficient Drosophila sensory neurons, which is dependent on Xbp1. Ringer is expressed in sensory neurons before and after injury, and is cell-autonomously required for axon regeneration. While loss of ringer abolishes the regeneration enhancement in Rtca mutants, its overexpression is sufficient to promote regeneration both in the peripheral and central nervous system. Ringer maintains microtubule stability/dynamics with the microtubule-associated protein futsch/MAP1B, which is also required for axon regeneration. Furthermore, ringer lies downstream from and is negatively regulated by the microtubule-associated deacetylase HDAC6, which functions as a regeneration inhibitor. Taken together, our findings suggest that ringer acts as a hub for microtubule regulators that relays cellular status information, such as cellular stress, to the integrity of microtubules in order to instruct neuroregeneration.
机译:在中枢和外周神经系统中促进轴突再生是神经损伤和神经变性疾病的临床重要性。正在识别既有和反寄售因子。我们之前报道的是RTCA介导的RNA修复/剪接途径通过抑制细胞应激下的XBP1 mRNA的非转化剪接来限制轴突再生。但是,下游效果仍然未知。这里,通过转录组分析,我们表明,在RTCA缺陷的果蝇感官神经元中,微管蛋白聚合促进蛋白(TPPP)圈状蛋白(TPPP)Ringmaker / Ringer在依赖于XBP1。 ringer在受伤前后的感觉神经元表达,并且是轴突再生所需的细胞自主。虽然失去ringer消除了RTCA突变体中的再生增强,但其过表达足以促进外周和中枢神经系统的再生。 Ringer将微管稳定性/动态与微管相关的蛋白FUTSCH / MAP1B保持,这也需要轴轴再生。此外,振铃器位于下游,并且由微管相关的脱乙酰酶HDAC6负调节,其用作再生抑制剂。我们的研究结果表明,ringer用作微管调节剂的枢纽,其将蜂窝状态信息(例如细胞应力)转移到微管的完整性,以指示神经循环。

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