Repeat associated mechanisms of genome evolution and function revealed by the Mus caroli and Mus pahari genomes.
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Authors
Thybert, David
Roller, Maša
Navarro, Fábio CP
Fiddes, Ian
Streeter, Ian
Martin-Galvez, David
Kolmogorov, Mikhail
Janoušek, Václav
Akanni, Wasiu
Aken, Bronwen
Aldridge, Sarah
Chakrapani, Varshith
Chow, William
Clarke, Laura
Cummins, Carla
Doran, Anthony
Dunn, Matthew
Goodstadt, Leo
Howe, Kerstin
Howell, Matthew
Josselin, Ambre-Aurore
Karn, Robert C
Laukaitis, Christina M
Jingtao, Lilue
Martin, Fergal
Muffato, Matthieu
Nachtweide, Stefanie
Quail, Michael A
Sisu, Cristina
Stanke, Mario
Stefflova, Klara
Van Oosterhout, Cock
Veyrunes, Frederic
Ward, Ben
Yang, Fengtang
Yazdanifar, Golbahar
Zadissa, Amonida
Adams, David J
Brazma, Alvis
Gerstein, Mark
Paten, Benedict
Pham, Son
Keane, Thomas M
Odom, Duncan T
Flicek, Paul
Publication Date
2018-04Journal Title
Genome Res
ISSN
1088-9051
Publisher
Cold Spring Harbor Laboratory
Volume
28
Issue
4
Pages
448-459
Language
eng
Type
Article
Physical Medium
Print-Electronic
Metadata
Show full item recordCitation
Thybert, D., Roller, M., Navarro, F. C., Fiddes, I., Streeter, I., Feig, C., Martin-Galvez, D., et al. (2018). Repeat associated mechanisms of genome evolution and function revealed by the Mus caroli and Mus pahari genomes.. Genome Res, 28 (4), 448-459. https://doi.org/10.1101/gr.234096.117
Abstract
Understanding the mechanisms driving lineage-specific evolution in both primates and rodents has been hindered by the lack of sister clades with a similar phylogenetic structure having high-quality genome assemblies. Here, we have created chromosome-level assemblies of the Mus caroli and Mus pahari genomes. Together with the Mus musculus and Rattus norvegicus genomes, this set of rodent genomes is similar in divergence times to the Hominidae (human-chimpanzee-gorilla-orangutan). By comparing the evolutionary dynamics between the Muridae and Hominidae, we identified punctate events of chromosome reshuffling that shaped the ancestral karyotype of Mus musculus and Mus caroli between 3 and 6 million yr ago, but that are absent in the Hominidae. Hominidae show between four- and sevenfold lower rates of nucleotide change and feature turnover in both neutral and functional sequences, suggesting an underlying coherence to the Muridae acceleration. Our system of matched, high-quality genome assemblies revealed how specific classes of repeats can play lineage-specific roles in related species. Recent LINE activity has remodeled protein-coding loci to a greater extent across the Muridae than the Hominidae, with functional consequences at the species level such as reproductive isolation. Furthermore, we charted a Muridae-specific retrotransposon expansion at unprecedented resolution, revealing how a single nucleotide mutation transformed a specific SINE element into an active CTCF binding site carrier specifically in Mus caroli, which resulted in thousands of novel, species-specific CTCF binding sites. Our results show that the comparison of matched phylogenetic sets of genomes will be an increasingly powerful strategy for understanding mammalian biology.
Keywords
Animals, Binding Sites, CCCTC-Binding Factor, Chromosomes, Evolution, Molecular, Genome, Karyotyping, Long Interspersed Nucleotide Elements, Mice, Muridae, Phylogeny, Retroelements, Species Specificity
Sponsorship
Cancer Research UK (C14303/A17197)
European Research Council (615584)
Cancer Research UK (20412)
Wellcome Trust (202878/Z/16/Z)
Identifiers
External DOI: https://doi.org/10.1101/gr.234096.117
This record's URL: https://www.repository.cam.ac.uk/handle/1810/279898
Rights
Attribution 4.0 International (CC BY 4.0)
Licence URL: https://creativecommons.org/licenses/by/4.0/
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