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Comprehensive identification of transposable element insertions using multiple sequencing technologies

Chong Chu, Rebeca Borges-Monroy, Vinay Viswanadham, Soohyun Lee, Heng Li, Eunjung Alice Lee, Peter J. Park

2021Nature Communications107 citationsDOIOpen Access PDF

Abstract

Transposable elements (TEs) help shape the structure and function of the human genome. When inserted into some locations, TEs may disrupt gene regulation and cause diseases. Here, we present xTea (x-Transposable element analyzer), a tool for identifying TE insertions in whole-genome sequencing data. Whereas existing methods are mostly designed for short-read data, xTea can be applied to both short-read and long-read data. Our analysis shows that xTea outperforms other short read-based methods for both germline and somatic TE insertion discovery. With long-read data, we created a catalogue of polymorphic insertions with full assembly and annotation of insertional sequences for various types of retroelements, including pseudogenes and endogenous retroviruses. Notably, we find that individual genomes have an average of nine groups of full-length L1s in centromeres, suggesting that centromeres and other highly repetitive regions such as telomeres are a significant yet unexplored source of active L1s. xTea is available at https://github.com/parklab/xTea .

Topics & Concepts

Transposable elementGenomePseudogeneBiologyComputational biologyGeneticsHuman genomeIndelCentromereRetrotransposonDNA sequencingGermlineGeneChromosomeSingle-nucleotide polymorphismGenotypeChromosomal and Genetic VariationsGenomics and Phylogenetic StudiesRNA and protein synthesis mechanisms
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