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高通量鉴定神经元细胞中的 RNA 定位元件。

High-throughput identification of RNA localization elements in neuronal cells.

机构信息

Department of Biochemistry and Molecular Genetics, University of Colorado Anschutz Medical Campus, USA.

Barbara Davis Center for Diabetes, University of Colorado Anschutz Medical Campus, USA.

出版信息

Nucleic Acids Res. 2022 Oct 14;50(18):10626-10642. doi: 10.1093/nar/gkac763.

Abstract

Hundreds of RNAs are enriched in the projections of neuronal cells. For the vast majority of them, though, the sequence elements that regulate their localization are unknown. To identify RNA elements capable of directing transcripts to neurites, we deployed a massively parallel reporter assay that tested the localization regulatory ability of thousands of sequence fragments drawn from endogenous mouse 3' UTRs. We identified peaks of regulatory activity within several 3' UTRs and found that sequences derived from these peaks were both necessary and sufficient for RNA localization to neurites in mouse and human neuronal cells. The localization elements were enriched in adenosine and guanosine residues. They were at least tens to hundreds of nucleotides long as shortening of two identified elements led to significantly reduced activity. Using RNA affinity purification and mass spectrometry, we found that the RNA-binding protein Unk was associated with the localization elements. Depletion of Unk in cells reduced the ability of the elements to drive RNAs to neurites, indicating a functional requirement for Unk in their trafficking. These results provide a framework for the unbiased, high-throughput identification of RNA elements and mechanisms that govern transcript localization in neurons.

摘要

数百种 RNA 存在于神经元细胞的投射物中。然而,对于其中绝大多数 RNA,调控其定位的序列元件尚不清楚。为了鉴定能够将转录本导向神经突的 RNA 元件,我们利用大规模平行报告基因检测方法,从内源性小鼠 3'UTR 中提取数千个序列片段,测试它们的定位调控能力。我们在几个 3'UTR 中发现了调控活性峰,并发现来自这些峰的序列在小鼠和人神经元细胞中对于 RNA 定位于神经突是必需和充分的。这些定位元件富含腺苷酸和鸟苷酸残基。它们至少有数十到数百个核苷酸长,因为两个鉴定出的元件缩短后会导致活性显著降低。利用 RNA 亲和纯化和质谱分析,我们发现 RNA 结合蛋白 Unk 与定位元件相关。细胞中 Unk 的耗竭降低了元件驱动 RNA 向神经突运输的能力,表明 Unk 在其运输过程中具有功能需求。这些结果为非偏见、高通量鉴定 RNA 元件以及调控神经元中转录物定位的机制提供了一个框架。

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