4.2 Article

Within-population Y-linked genetic variation for lifespan in Drosophila melanogaster

Journal

JOURNAL OF EVOLUTIONARY BIOLOGY
Volume 28, Issue 11, Pages 1940-1947

Publisher

WILEY
DOI: 10.1111/jeb.12708

Keywords

intralocus sexual conflict; longevity; sex chromosomes; sexual dimorphism; Y chromosome

Funding

  1. Swedish Foundation for Strategic Research
  2. Carl Tryggers Foundation
  3. Swedish Research Council
  4. German Research Foundation (DFG) [SCHI 1188/1-1]

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The view that the Y chromosome is of little importance for phenotypic evolution stems from early studies of Drosophila melanogaster. This species' Y chromosome contains only 13 protein-coding genes, is almost entirely heterochromatic and is not necessary for male viability. Population genetic theory further suggests that non-neutral variation can only be maintained at the Y chromosome under special circumstances. Yet, recent studies suggest that the D.melanogaster Y chromosome trans-regulates hundreds to thousands of X and autosomal genes. This finding suggests that the Y chromosome may play a far more active role in adaptive evolution than has previously been assumed. To evaluate the potential for the Y chromosome to contribute to phenotypic evolution from standing genetic variation, we test for Y-linked variation in lifespan within a population of D.melanogaster. Assessing variation for lifespan provides a powerful test because lifespan (i) shows sexual dimorphism, which the Y is primarily predicted to contribute to, (ii) is influenced by many genes, which provides the Y with many potential regulatory targets and (iii) is sensitive to heterochromatin remodelling, a mechanism through which the Y chromosome is believed to regulate gene expression. Our results show a small but significant effect of the Y chromosome and thus suggest that the Y chromosome has the potential to respond to selection from standing genetic variation. Despite its small effect size, Y-linked variation may still be important, in particular when evolution of sexual dimorphism is genetically constrained elsewhere in the genome.

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