Genomic impact of eukaryotic transposable elements

Cells, 2022

Transposable elements (TEs) are ubiquitous genetic elements, able to jump from one location of the genome to another, in all organisms. For this reason, on the one hand, TEs can induce deleterious mutations, causing dysfunction, disease and even lethality in individuals. On the other hand, TEs can increase genetic variability, making populations better equipped to respond adaptively to environmental change. To counteract the deleterious effects of TEs, organisms have evolved strategies to avoid their activation. However, their mobilization does occur. Usually, TEs are maintained silent through several mechanisms, but they can be reactivated during certain developmental windows. Moreover, TEs can become de-repressed because of drastic changes in the external environment. Here, we describe the ‘double life’ of TEs, being both ‘parasites’ and ‘symbionts’ of the genome. We also argue that the transposition of TEs contributes to two important evolutionary processes: the temporal dynamic ...

NATO Science for Peace and Security Series C: Environmental Security, 2011

Transposable elements (TEs) are selfi sh fragments of DNA able to reproduce themselves into the host genomes. TEs typically occupy ~40-50% of the mammalian genomes. In our studies, we focus on evolutionary recent TE inserts that appeared in the DNA of human ancestor lineage after divergence with the chimpanzee ancestry, i.e. less than ~6 million years ago. These human specifi c elements (hsTEs) represent only a minor fraction of the whole TE cargo of the human genome. hsTEs are represented by the four families called HERV-K(HML-2), L1, Alu and SVA. The number of human specifi c copies for HERV-K(HML-2), L1, Alu and SVA families is approx. 150, 1,200, 5,500 and 860 copies per genome, respectively. Taken together, hsTEs shape ~6.4 megabases of human DNA, which is about 6-times lower than what is occupied by the human specifi c simple nucleotide polymorphisms, and 23-times smaller than the overall length of human specifi c deletions and duplications. However, although modest in terms of genomic proportion, hsTEs should be regarded as the perspective candidates for being molecular genetic agents of human speciation. Unlike most of random mutations and duplications, each novel insert of hsTE has provided to the recipient genomic locus a set of functional transcriptional factor binding sites positively selected during the TE evolution. For example, clusters of novel inserts of Alu elements may serve as CpG islets, SVA elements provide functional splice sites and polyadenylation signals, whereas L1 and HERV-K(HML-2) elements donate enhancers, promoters, splice sites and polyadenylation signals. Signifi cant proportion of the human-specifi c genomic deletions,

Trends in Genetics, 2003

Nature Reviews Genetics, 2007

| Our knowledge of the structure and composition of genomes is rapidly progressing in pace with their sequencing. The emerging data show that a significant portion of eukaryotic genomes is composed of transposable elements (TEs). Given the abundance and diversity of TEs and the speed at which large quantities of sequence data are emerging, identification and annotation of TEs presents a significant challenge. Here we propose the first unified hierarchical classification system, designed on the basis of the transposition mechanism, sequence similarities and structural relationships, that can be easily applied by non-experts. The system and nomenclature is kept up to date at the WikiPoson web site.

Nucleic Acids Research, 2014

Transposable elements (TEs) are the most active, diverse and ancient component 42 in a broad range of genomes. As such, a complete understanding of genome function 43 and evolution cannot be achieved without a thorough understanding of TE impact and 44 biology. However, in-depth analyses of TEs still represent a challenge due to the 45 repetitive nature of these genomic entities. In this work, we present a broadly applicable 46 and flexible tool: T-lex2. T-lex2 is the only available software that allows routine, 47 automatic, and accurate genotyping of individual TE insertions and estimation of their 48 population frequencies both using individual strain and pooled next-generation 49 sequencing (NGS) data. Furthermore, T-lex2 also assesses the quality of the calls 50 allowing the identification of miss-annotated TEs and providing the necessary 51 information to re-annotate them. Although we tested the fidelity of T-lex2 using the high 52 quality Drosophila melanogaster genome, the flexible and customizable design of T-53 lex2 allows running it in any genome and for any type of TE insertion. Overall, T-lex2 54 represents a significant improvement in our ability to analyze the contribution of TEs to 55 genome function and evolution as well as learning about the biology of TEs. T-lex2 is 56 freely available online at http://petrov.stanford.edu/cgi-bin/Tlex.html. 57 58 on October 20, 2014 http://biorxiv.org/ Downloaded from 59 60

Nature Reviews Genetics, 2011

Transposable elements (TEs) have a unique ability to mobilize to new genomic locations and the major advance of next-generation DNA sequencing has provided insights into the dynamic relationship between TEs and their hosts. It now is clear that TEs have adopted diverse strategiessuch as specific integration sites or patterns of activity -to thrive in host environments that are replete with mechanisms -such as small RNAs or epigenetic marks -to combat their amplification. Emerging evidence suggests that TE mobilization might sometimes benefit host genomes by enhancing genetic diversity, but TEs are also implicated in diseases such as cancer.

Mobile genetic elements, 2017

Recent technological developments-in genomics, bioinformatics and high-throughput experimental techniques-are providing opportunities to study ongoing human transposable element (TE) activity at an unprecedented level of detail. It is now possible to characterize genome-wide collections of TE insertion sites for multiple human individuals, within and between populations, and for a variety of tissue types. Comparison of TE insertion site profiles between individuals captures the germline activity of TEs and reveals insertion site variants that segregate as polymorphisms among human populations, whereas comparison among tissue types ascertains somatic TE activity that generates cellular heterogeneity. In this review, we provide an overview of these new technologies and explore their implications for population and clinical genetic studies of human TEs. We cover both recent published results on human TE insertion activity as well as the prospects for future TE studies related to human ...

EMBO reports, 2009

EMBO reports, 2009

the summer research conference on Mobile Elements in Mammalian genomes took place between 5 and 10 July 2009 in Snowmass Village, colorado, uSa, and was organized by S. Martin, g.g. Schumann and p. Deininger. photo credit: Deborah Bourc'his.

International Journal of Molecular Sciences

Transposable elements (TEs), which cover ~45% of the human genome, although firstly considered as “selfish” DNA, are nowadays recognized as driving forces in eukaryotic genome evolution. This capability resides in generating a plethora of sophisticated RNA regulatory networks that influence the cell type specific transcriptome in health and disease. Indeed, TEs are transcribed and their RNAs mediate multi-layered transcriptional regulatory functions in cellular identity establishment, but also in the regulation of cellular plasticity and adaptability to environmental cues, as occurs in the immune response. Moreover, TEs transcriptional deregulation also evolved to promote pathogenesis, as in autoimmune and inflammatory diseases and cancers. Importantly, many of these findings have been achieved through the employment of Next Generation Sequencing (NGS) technologies and bioinformatic tools that are in continuous improvement to overcome the limitations of analyzing TEs sequences. Howe...