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体内基因表达的研究:增强型双色荧光转录时标

In vivo study of gene expression with an enhanced dual-color fluorescent transcriptional timer.

机构信息

Department of Genetics, Harvard Medical School, Boston, United States.

Howard Hughes Medical Institute, Boston, United States.

出版信息

Elife. 2019 May 29;8:e46181. doi: 10.7554/eLife.46181.

Abstract

Fluorescent transcriptional reporters are widely used as signaling reporters and biomarkers to monitor pathway activities and determine cell type identities. However, a large amount of dynamic information is lost due to the long half-life of the fluorescent proteins. To better detect dynamics, fluorescent transcriptional reporters can be destabilized to shorten their half-lives. However, applications of this approach in vivo are limited due to significant reduction of signal intensities. To overcome this limitation, we enhanced translation of a destabilized fluorescent protein and demonstrate the advantages of this approach by characterizing spatio-temporal changes of transcriptional activities in . In addition, by combining a fast-folding destabilized fluorescent protein and a slow-folding long-lived fluorescent protein, we generated a dual-color transcriptional timer that provides spatio-temporal information about signaling pathway activities. Finally, we demonstrate the use of this transcriptional timer to identify new genes with dynamic expression patterns.

摘要

荧光转录报告基因广泛用作信号报告基因和生物标志物,用于监测途径活性和确定细胞类型。然而,由于荧光蛋白的半衰期长,大量的动态信息丢失。为了更好地检测动态变化,可以使荧光转录报告基因失稳以缩短其半衰期。然而,由于信号强度的显著降低,该方法在体内的应用受到限制。为了克服这一限制,我们增强了不稳定荧光蛋白的翻译,并通过对. 中转录活性的时空变化进行表征来证明该方法的优势。此外,通过结合快速折叠失稳荧光蛋白和缓慢折叠长寿命荧光蛋白,我们生成了一个双色转录计时器,提供了关于信号通路活性的时空信息。最后,我们证明了使用这种转录计时器来识别具有动态表达模式的新基因。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0953/6660218/456ebc0072f4/elife-46181-fig1.jpg

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