Abstract

Genome evolution is driven by the activity of transposable elements (TEs). The spread of TEs can have deleterious effects including the destabilization of genome integrity and expansions. However, the precise triggers of genome expansions remain poorly understood because genome size evolution is typically investigated only among deeply divergent lineages. Here, we use a large population genomics dataset of 284 individuals from populations across the globe of Zymoseptoria tritici, a major fungal wheat pathogen. We built a robust map of genome-wide TE insertions and deletions to track a total of 2456 polymorphic loci within the species. We show that purifying selection substantially depressed TE frequencies in most populations, but some rare TEs have recently risen in frequency and likely confer benefits. We found that specific TE families have undergone a substantial genome-wide expansion from the pathogen's center of origin to more recently founded populations. The most dramatic increase in TE insertions occurred between a pair of North American populations collected in the same field at an interval of 25 years. We find that both genome-wide counts of TE insertions and genome size have increased with colonization bottlenecks. Hence, the demographic history likely played a major role in shaping genome evolution within the species. We show that both the activation of specific TEs and relaxed purifying selection underpin this incipient expansion of the genome. Our study establishes a model to recapitulate TE-driven genome evolution over deeper evolutionary timescales.

Highlights

  • Transposable elements (TEs) are mobile repetitive DNA sequences with the ability to independently insert into new regions of the genome

  • We found robust evidence for a total of 18,864 TE insertions grouping into 2465 individual loci

  • TEs play a crucial role in generating adaptive genetic variation within species but are drivers of deleterious genome expansions

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Summary

Introduction

Transposable elements (TEs) are mobile repetitive DNA sequences with the ability to independently insert into new regions of the genome. Insertion of TEs can disrupt coding sequences, trigger chromosomal rearrangements, or alter expression profiles of adjacent genes (Lim, 1988; Petrov et al, 2003; Slotkin and Martienssen, 2007; Hollister and Gaut, 2009; Oliver et al, 2013). TE activity can have phenotypic consequences and impact host fitness. While TE insertion dynamics are driven by the selfish interest for proliferation, the impact on the host can range from beneficial to highly deleterious. The most dramatic examples of TE insertions underpinned rapid adaptation of populations or species (Feschotte, 2008; Chuong et al, 2017),

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