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. 2008;9(2):R30.
doi: 10.1186/gb-2008-9-2-r30. Epub 2008 Feb 12.

Genomic degradation of a young Y chromosome in Drosophila miranda

Doris Bachtrog  1 Emily HomKaren M WongXulio MasidePieter de Jong
Affiliations

Genomic degradation of a young Y chromosome in Drosophila miranda

Doris Bachtrog et al. Genome Biol. 2008.

Abstract

Background: Y chromosomes are derived from ordinary autosomes and degenerate because of a lack of recombination. Well-studied Y chromosomes only have few of their original genes left and contain little information about their evolutionary origin. Here, we take advantage of the recently formed neo-Y chromosome of Drosophila miranda to study the processes involved in Y degeneration on a genomic scale.

Results: We obtained sequence information from 14 homologous bacterial artificial chromosome (BAC) clones from the neo-X and neo-Y chromosome of D. miranda, encompassing over 2.5 Mb of neo-sex-linked DNA. A large fraction of neo-Y DNA is composed of repetitive and transposable-element-derived DNA (20% of total DNA) relative to their homologous neo-X linked regions (1%). The overlapping regions of the neo-sex linked BAC clones contain 118 gene pairs, half of which are pseudogenized on the neo-Y. Pseudogenes evolve significantly faster on the neo-Y than functional genes, and both functional and non-functional genes show higher rates of protein evolution on the neo-Y relative to their neo-X homologs. No heterogeneity in levels of degeneration was detected among the regions investigated. Functional genes on the neo-Y are under stronger evolutionary constraint on the neo-X, but genes were found to degenerate randomly on the neo-Y with regards to their function or sex-biased expression patterns.

Conclusion: Patterns of genome evolution in D. miranda demonstrate that degeneration of a recently formed Y chromosome can proceed very rapidly, by both an accumulation of repetitive DNA and degeneration of protein-coding genes. Our data support a random model of Y inactivation, with little heterogeneity in degeneration among genomic regions, or between functional classes of genes or genes with sex-biased expression patterns.

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Figures

Figure 1
Figure 1
Schematic overview of the genomic regions investigated on the neo-sex chromosomes, anchored on the D. pseudoobscura genomic annotation. Genes in grey represent pseudogenes on the neo-Y.
See this image and copyright information in PMC

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