4.8 Article

Genome expansion via lineage splitting and genome reduction in the cicada endosymbiont Hodgkinia

Publisher

NATL ACAD SCIENCES
DOI: 10.1073/pnas.1421386112

Keywords

symbiosis; genome evolution; nonadaptive evolution; organelles; bacteria

Funding

  1. National Institutes of Health National Institute of General Medical Sciences [P20RR017670]
  2. M. J. Murdock Charitable Trust
  3. National Science Foundation [DEB-0955849, DEB-0529679, IOS-1256680]
  4. NSF-EPSCoR [NSF-IIA-1443108]
  5. National Aeronautics and Space Administration Astrobiology Institute [NNA15BB04A]
  6. Direct For Biological Sciences
  7. Division Of Environmental Biology [0955849] Funding Source: National Science Foundation
  8. Office Of The Director
  9. Office of Integrative Activities [1443108] Funding Source: National Science Foundation

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Comparative genomics from mitochondria, plastids, and mutualistic endosymbiotic bacteria has shown that the stable establishment of a bacterium in a host cell results in genome reduction. Although many highly reduced genomes from endosymbiotic bacteria are stable in gene content and genome structure, organelle genomes are sometimes characterized by dramatic structural diversity. Previous results from Candidatus Hodgkinia cicadicola, an endosymbiont of cicadas, revealed that some lineages of this bacterium had split into two new cytologically distinct yet genetically interdependent species. It was hypothesized that the long life cycle of cicadas in part enabled this unusual lineage-splitting event. Here we test this hypothesis by investigating the structure of the Ca. Hodgkinia genome in one of the longest-lived cicadas, Magicicada tredecim. We show that the Ca. Hodgkinia genome from M. tredecim has fragmented into multiple new chromosomes or genomes, with at least some remaining partitioned into discrete cells. We also show that this lineage-splitting process has resulted in a complex of Ca. Hodgkinia genomes that are 1.1-Mb pairs in length when considered together, an almost 10-fold increase in size from the hypothetical single-genome ancestor. These results parallel some examples of genome fragmentation and expansion in organelles, although the mechanisms that give rise to these extreme genome instabilities are likely different.

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