Identification of EMS-induced mutations in Drosophila melanogaster by whole-genome sequencing

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Abstract

Next-generation methods for rapid whole-genome sequencing enable the identification of single-base-pair mutations in Drosophila by comparing a chromosome bearing a new mutation to the unmutagenized sequence. To validate this approach, we sought to identify the molecular lesion responsible for a recessive EMS-induced mutation affecting egg shell morphology by using Illumina next-generation sequencing. After obtaining sufficient sequence from larvae that were homozygous for either wild-type or mutant chromosomes, we obtained high-quality reads for base pairs composing ∼70% of the third chromosome of both DNA samples. We verified 103 single-base-pair changes between the two chromosomes. Nine changes were nonsynonymous mutations and two were nonsense mutations. One nonsense mutation was in a gene, encore, whose mutations produce an egg shell phenotype also observed in progeny of homozygous mutant mothers. Complementation analysis revealed that the chromosome carried a new functional allele of encore, demonstrating that one round of next-generation sequencing can identify the causative lesion for a phenotype of interest. This new method of whole-genome sequencing represents great promise for mutant mapping in flies, potentially replacing conventional methods. Copyright © 2009 by the Genetics Society of America.

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Blumenstiel, J. P., Noll, A. C., Griffiths, J. A., Perera, A. G., Walton, K. N., Gilliland, W. D., … Staehling-Hampton, K. (2009). Identification of EMS-induced mutations in Drosophila melanogaster by whole-genome sequencing. Genetics, 182(1), 25–32. https://doi.org/10.1534/genetics.109.101998

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