转座元件有助于人类组织特异性基因调控。

Transposable elements contribute to tissue-specific gene regulation in humans.

机构信息

Department of Biological Sciences, Brock University, St. Catharines, ON, L2S 3A1, Canada.

Centre of Biotechnologies, Brock University, St. Catharines, ON, L2S 3A1, Canada.

出版信息

Genes Genomics. 2024 Nov;46(11):1327-1343. doi: 10.1007/s13258-024-01550-6. Epub 2024 Aug 1.

DOI:10.1007/s13258-024-01550-6

PMID:39088190

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11602805/

Abstract

BACKGROUND

Transposable elements (TEs) contribute to approximately half of the human genome, and along with many other functions, they have been known to play a role in gene regulation in the genome. With TEs' active/repressed states varying across tissue and cell types, they have the potential to regulate gene expression in a tissue-specific manner.

OBJECTIVE AND METHODS

To provide a systematic analysis of TEs' contribution in tissue-specific gene regulation, we examined the regulatory elements and genes in association with TE-derived regulatory sequences in 14 human cell lines belonging to 10 different tissue types using the functional genomics data from the ENCODE project. Specifically, we separately analyzed regulatory regions identified by three different approaches (DNase hypersensitive sites (DHS), histone active sites (HA), and histone repressive sites (HR)).

RESULTS

These regulatory regions showed to be distinct from each other by sharing less than 2.5% among all three types and more than 95% showed to be cell line-specific. Despite a lower total TE content overall than the genome average, each regulatory sequence type showed enrichment for one or two specific TE type(s): DHS for long terminal repeats (LTRs) and DNA transposons, HA for short interspersed nucleotide elements (SINEs), and HR for LTRs. In contrast, SINE was shown to be overrepresented in all three types of regulatory sequences located in gene-neighboring regions. TE-regulated genes were mostly shown to have cell line specific pattern, and tissue-specific genes (TSGs) showed higher usage of TE regulatory sequences in the tissue of their expression. While TEs in the regulatory sequences showed to be older than their genome-wide counterparts, younger TEs were shown to be more likely used in cell line specific regulatory sequences.

CONCLUSIONS

Collectively, our study provided further evidence enforcing an important contribution of TEs to tissue-specific gene regulation in humans.

摘要

背景

转座元件（TEs）约占人类基因组的一半，除了许多其他功能外，它们还被认为在基因组基因调控中发挥作用。由于 TEs 的活跃/抑制状态在组织和细胞类型中各不相同，它们有可能以组织特异性的方式调节基因表达。

目的和方法

为了系统分析 TEs 在组织特异性基因调控中的作用，我们利用 ENCODE 项目的功能基因组学数据，检查了 14 个人类细胞系（属于 10 种不同组织类型）中与 TE 衍生调节序列相关的调节元件和基因。具体来说，我们分别分析了三种不同方法（DNase 敏感位点（DHS）、组蛋白活性位点（HA）和组蛋白抑制性位点（HR））识别的调节区域。

结果

这些调节区域彼此之间的共享不到 2.5%，而超过 95%的区域表现出细胞系特异性。尽管每种调节序列类型的总 TE 含量总体上低于基因组平均值，但每种类型的调节序列都富集了一种或两种特定的 TE 类型：DHS 为长末端重复（LTR）和 DNA 转座子，HA 为短散在核元件（SINE），HR 为 LTR。相比之下，SINE 在所有三种位于基因邻近区域的调节序列类型中都表现出过度表达。TE 调节基因主要表现出细胞系特异性模式，组织特异性基因（TSGs）在其表达的组织中使用更多的 TE 调节序列。虽然调节序列中的 TE 比其全基因组对应物更古老，但年轻的 TE 更有可能被用于细胞系特异性调节序列。