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capTEs 能够实现从参考和非参考转座元件中对转录产物进行特定基因座的剖析。

capTEs enables locus-specific dissection of transcriptional outputs from reference and nonreference transposable elements.

机构信息

Laboratory of Omics Technology and Bioinformatics, Frontiers Science Center for Disease-related Molecular Network, State Key Laboratory of Biotherapy, West China Hospital, Sichuan University, Chengdu, Sichuan, 610041, China.

出版信息

Commun Biol. 2023 Sep 23;6(1):974. doi: 10.1038/s42003-023-05349-1.

Abstract

Transposable elements (TEs) serve as both insertional mutagens and regulatory elements in cells, and their aberrant activity is increasingly being revealed to contribute to diseases and cancers. However, measuring the transcriptional consequences of nonreference and young TEs at individual loci remains challenging with current methods, primarily due to technical limitations, including short read lengths generated and insufficient coverage in target regions. Here, we introduce a long-read targeted RNA sequencing method, Cas9-assisted profiling TE expression sequencing (capTEs), for quantitative analysis of transcriptional outputs for individual TEs, including transcribed nonreference insertions, noncanonical transcripts from various transcription patterns and their correlations with expression changes in related genes. This method selectively identified TE-containing transcripts and outputted data with up to 90% TE reads, maintaining a comparable data yield to whole-transcriptome sequencing. We applied capTEs to human cancer cells and found that internal and inserted Alu elements may employ distinct regulatory mechanisms to upregulate gene expression. We expect that capTEs will be a critical tool for advancing our understanding of the biological functions of individual TEs at the locus level, revealing their roles as both mutagens and regulators in biological and pathogenic processes.

摘要

转座元件 (TEs) 在细胞中既是插入突变因子,又是调节元件,它们的异常活性越来越多地被揭示与疾病和癌症有关。然而,由于技术限制,包括生成的短读长和目标区域的覆盖不足,目前的方法仍然难以测量非参考和年轻 TEs 在单个基因座上的转录后果。在这里,我们引入了一种长读长靶向 RNA 测序方法,Cas9 辅助分析 TE 表达测序 (capTEs),用于定量分析单个 TE 的转录产物,包括转录的非参考插入物、来自各种转录模式的非规范转录本及其与相关基因表达变化的相关性。该方法选择性地识别包含 TE 的转录本,并输出高达 90%TE 读数的数据,与全转录组测序相比保持相当的数据产量。我们将 capTEs 应用于人类癌细胞,并发现内部和插入的 Alu 元件可能采用不同的调节机制来上调基因表达。我们预计 capTEs 将成为推进我们在基因座水平上理解单个 TE 的生物学功能的重要工具,揭示它们在生物和病理过程中既是突变因子又是调节因子的作用。

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