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首页> 外文期刊>Cell Regeneration >Loss of Mgat5a-mediated N-glycosylation stimulates regeneration in zebrafish
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Loss of Mgat5a-mediated N-glycosylation stimulates regeneration in zebrafish

机译:Mgat5a介导的N-糖基化的损失刺激斑马鱼的再生。

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Abstract Background We are using genetics to identify genes specifically involved in hearing regeneration. In a large-scale genetic screening, we identified mgat5a, a gene in the N-glycosylation biosynthesis pathway whose activity negatively impacts hair cell regeneration. Methods We used a combination of mutant analysis in zebrafish and a hair cell regeneration assay to phenotype the loss of Mgat5a activity in zebrafish. We used pharmacological inhibition of N-glycosylation by swansonine. We also used over-expression analysis by mRNA injections to demonstrate how changes in N-glycosylation can alter cell signaling. Results We found that mgat5a was expressed in multiple tissues during zebrafish embryo development, particularly enriched in neural tissues including the brain, retina, and lateral line neuromasts. An mgat5a insertional mutation and a CRISPR/Cas9-generated truncation mutation both caused an enhancement of hair cell regeneration which could be phenocopied by pharmacological inhibition with swansonine. In addition to hair cell regeneration, inhibition of the N-glycosylation pathway also enhanced the regeneration of lateral line axon and caudal fins. Further analysis showed that N-glycosylation altered the responsiveness of TGF-beta signaling. Conclusions The findings from this study provide experimental evidence for the involvement of N-glycosylation in tissue regeneration and cell signaling.
机译:摘要背景我们正在使用遗传学来鉴定专门与听力再生有关的基因。在大规模的遗传筛选中,我们鉴定了mgat5a,它是N-糖基化生物合成途径中的一个基因,其活性对毛细胞的再生产生负面影响。方法我们结合使用了斑马鱼中的突变分析和毛细胞再生分析来对斑马鱼中Mgat5a活性的丧失进行表型分析。我们使用了斯旺森碱对N-糖基化的药理抑制作用。我们还使用了通过mRNA注射进行的过表达分析,以证明N-糖基化的变化如何改变细胞信号传导。结果我们发现mgat5a在斑马鱼胚胎发育过程中在多种组织中表达,特别是在包括脑,视网膜和侧线神经质的神经组织中富集。 mgat5a插入突变和CRISPR / Cas9产生的截短突变均引起毛细胞再生增强,这可以通过用swansonine进行药理学抑制而表现出来。除毛细胞再生外,抑制N-糖基化途径还增强了侧线轴突和尾鳍的再生。进一步的分析表明,N-糖基化改变了TGF-β信号传导的响应能力。结论该研究的发现为N-糖基化参与组织再生和细胞信号传导提供了实验证据。

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