Publication

Meeting our Makers:Uncovering the cis-regulatory activity of transposable elements using statistical learning

Abstract

The adaptation of organisms to their environment depends on the innovative potential inherent to genetic variation. In complex organisms such as mammals, processes like development and immunity require tight gene regulation. Complex forms emerge more often as a result of changes in gene regulation rather than gene products. Recent evidence accumulates to suggest that after spreading, transposable elements may become co-opted as cis-regulatory elements, thereby integrating neighboring genes into gene regulatory networks. Current methods for detecting cis-regulatory transposable elements rely on the joint exploration of multi-omics datasets, whose generation is both costly and time-consuming. We propose that modeling protein-coding gene expression (RNA-seq) as a function of the distribution of transposable elements into subfamilies as well as their respective genomic distances to promoters is sufficient to detect changes in transposable element-mediated cis-regulation. We leverage this model to show that far from solely affecting transcription during pre-implantation embryogenesis, evolutionarily recent transposable elements fine tune gene expression in cis throughout and beyond gastrulation while controlled by conserved master transcription factors. Moreover, we find that transposable elements optimally explain transcription at protein-coding gene promoters located within a 500kb range. Altogether, this work quantitatively shows that transposable elements disperse ready-for-use cis-acting platforms poised for integrating genes into regulatory networks controlled by conserved transcriptional and epigenetic regulators. Thus, metazoan adaptation appears to emerge from a rich genomic ecosystem whereby transposable elements propagate in the gene pool in symbiosis with their cognate activators and controllers. Methods-wise, our work opens up new avenues for studying the regulatory role of transposable elements in the next-generation sequencing era.

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Related concepts (35)
Cis-regulatory element
Cis-regulatory elements (CREs) or Cis''-regulatory modules (CRMs) are regions of non-coding DNA which regulate the transcription of neighboring genes. CREs are vital components of genetic regulatory networks, which in turn control morphogenesis, the development of anatomy, and other aspects of embryonic development, studied in evolutionary developmental biology. CREs are found in the vicinity of the genes that they regulate. CREs typically regulate gene transcription by binding to transcription factors.
Gene expression
Gene expression is the process by which information from a gene is used in the synthesis of a functional gene product that enables it to produce end products, proteins or non-coding RNA, and ultimately affect a phenotype. These products are often proteins, but in non-protein-coding genes such as transfer RNA (tRNA) and small nuclear RNA (snRNA), the product is a functional non-coding RNA.
Regulation of gene expression
Regulation of gene expression, or gene regulation, includes a wide range of mechanisms that are used by cells to increase or decrease the production of specific gene products (protein or RNA). Sophisticated programs of gene expression are widely observed in biology, for example to trigger developmental pathways, respond to environmental stimuli, or adapt to new food sources. Virtually any step of gene expression can be modulated, from transcriptional initiation, to RNA processing, and to the post-translational modification of a protein.
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