Local assembly of long reads enables phylogenomics of transposable elements in a polyploid cell line

Author:

Han Shunhua1ORCID,Dias Guilherme B12ORCID,Basting Preston J1ORCID,Viswanatha Raghuvir3ORCID,Perrimon Norbert34ORCID,Bergman Casey M12ORCID

Affiliation:

1. Institute of Bioinformatics, University of Georgia , 120 E. Green St., Athens, GA, USA

2. Department of Genetics, University of Georgia , 120 E. Green St., Athens, GA, USA

3. Department of Genetics, Harvard Medical School , 77 Avenue Louis Pasteur, Boston, MA, USA

4. Howard Hughes Medical Institute , Boston, MA, USA

Abstract

Abstract Animal cell lines often undergo extreme genome restructuring events, including polyploidy and segmental aneuploidy that can impede de novo whole-genome assembly (WGA). In some species like Drosophila, cell lines also exhibit massive proliferation of transposable elements (TEs). To better understand the role of transposition during animal cell culture, we sequenced the genome of the tetraploid Drosophila S2R+ cell line using long-read and linked-read technologies. WGAs for S2R+ were highly fragmented and generated variable estimates of TE content across sequencing and assembly technologies. We therefore developed a novel WGA-independent bioinformatics method called TELR that identifies, locally assembles, and estimates allele frequency of TEs from long-read sequence data (https://github.com/bergmanlab/telr). Application of TELR to a ∼130x PacBio dataset for S2R+ revealed many haplotype-specific TE insertions that arose by transposition after initial cell line establishment and subsequent tetraploidization. Local assemblies from TELR also allowed phylogenetic analysis of paralogous TEs, which revealed that proliferation of TE families in vitro can be driven by single or multiple source lineages. Our work provides a model for the analysis of TEs in complex heterozygous or polyploid genomes that are recalcitrant to WGA and yields new insights into the mechanisms of genome evolution in animal cell culture.

Funder

University of Georgia Research Education

Howard Hughes Medical Institute

Human Frontiers of Science Program

Georgia Research Foundation

Publisher

Oxford University Press (OUP)

Subject

Genetics

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