Genomic Rearrangements in Arabidopsis Considered as Quantitative Traits

Author:

Imprialou Martha12,Kahles André3,Steffen Joshua G4,Osborne Edward J4,Gan Xiangchao5,Lempe Janne5,Bhomra Amarjit1,Belfield Eric6,Visscher Anne67,Greenhalgh Robert4,Harberd Nicholas P6,Goram Richard8,Hein Jotun2,Robert-Seilaniantz Alexandre9,Jones Jonathan10,Stegle Oliver11,Kover Paula12,Tsiantis Miltos5,Nordborg Magnus13,Rätsch Gunnar3,Clark Richard M414,Mott Richard15

Affiliation:

1. Wellcome Trust Centre for Human Genetics, University of Oxford, OX3 7BN, United Kingdom

2. Department of Statistics, University of Oxford, OX1 3TG, United Kingdom

3. Department of Computer Science, Swiss Federal Institute of Technology in Zurich, 8092, Switzerland

4. Department of Biology, University of Utah, Salt Lake City, Utah 84112-0840

5. Department of Comparative Development and Genetics, Max Planck Institute for Plant Breeding Research, 50829 Köln, Germany

6. Department of Plant Sciences, University of Oxford, OX1 3RB, United Kingdom

7. Department of Comparative Plant and Fungal Biology, Royal Botanic Gardens Kew, Ardingly RH17 6TN, United Kingdom

8. John Innes Centre, Norwich NR4 7UH, United Kingdom

9. UMR INRA-Agrocampus Ouest-Université de Rennes 1, 35653 Le Rheu Cedex, France

10. The Sainsbury Laboratory, Norwich Research Park, NR4 7UH, United Kingdom

11. European Bioinformatics Institute, Hinxton, Cambridge CB10 1SD, United Kingdom

12. Department of Biology and Biochemistry, University of Bath, BA2 7AY, United Kingdom

13. Department of Population Genetics, Gregor Mendel Institute of Molecular Plant Biology, 1030 Vienna, Austria

14. Center for Cell and Genome Science, University of Utah, Salt Lake City, Utah 84112-0840

15. UCL Genetics Institute, University College London, WC1 6BT, United Kingdom

Abstract

Abstract Structural Rearrangements can have unexpected effects on quantitative phenotypes. Surprisingly, these rearrangements can also be considered as... To understand the population genetics of structural variants and their effects on phenotypes, we developed an approach to mapping structural variants that segregate in a population sequenced at low coverage. We avoid calling structural variants directly. Instead, the evidence for a potential structural variant at a locus is indicated by variation in the counts of short-reads that map anomalously to that locus. These structural variant traits are treated as quantitative traits and mapped genetically, analogously to a gene expression study. Association between a structural variant trait at one locus, and genotypes at a distant locus indicate the origin and target of a transposition. Using ultra-low-coverage (0.3×) population sequence data from 488 recombinant inbred Arabidopsis thaliana genomes, we identified 6502 segregating structural variants. Remarkably, 25% of these were transpositions. While many structural variants cannot be delineated precisely, we validated 83% of 44 predicted transposition breakpoints by polymerase chain reaction. We show that specific structural variants may be causative for quantitative trait loci for germination and resistance to infection by the fungus Albugo laibachii, isolate Nc14. Further we show that the phenotypic heritability attributable to read-mapping anomalies differs from, and, in the case of time to germination and bolting, exceeds that due to standard genetic variation. Genes within structural variants are also more likely to be silenced or dysregulated. This approach complements the prevalent strategy of structural variant discovery in fewer individuals sequenced at high coverage. It is generally applicable to large populations sequenced at low-coverage, and is particularly suited to mapping transpositions.

Publisher

Oxford University Press (OUP)

Subject

Genetics

Reference51 articles.

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