Volume 72, Issue 3 p. 568-577
ORIGINAL ARTICLE

Sex differences in life span: Females homozygous for the X chromosome do not suffer the shorter life span predicted by the unguarded X hypothesis

Martin Brengdahl,

IFM Biology, AVIAN Behavioural Genomics and Physiology Group, Linköping University, Linköping, Sweden

MB and CMK should be considered joint first author.

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Christopher M. Kimber,

IFM Biology, AVIAN Behavioural Genomics and Physiology Group, Linköping University, Linköping, Sweden

MB and CMK should be considered joint first author.

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Jack Maguire-Baxter,

IFM Biology, AVIAN Behavioural Genomics and Physiology Group, Linköping University, Linköping, Sweden

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Urban Friberg,

IFM Biology, AVIAN Behavioural Genomics and Physiology Group, Linköping University, Linköping, Sweden

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First published: 12 February 2018
Citations: 5

Abstract

Life span differs between the sexes in many species. Three hypotheses to explain this interesting pattern have been proposed, involving different drivers: sexual selection, asymmetrical inheritance of cytoplasmic genomes, and hemizygosity of the X(Z) chromosome (the unguarded X hypothesis). Of these, the unguarded X has received the least experimental attention. This hypothesis suggests that the heterogametic sex suffers a shortened life span because recessive deleterious alleles on its single X(Z) chromosome are expressed unconditionally. In Drosophila melanogaster, the X chromosome is unusually large (∼20% of the genome), providing a powerful model for evaluating theories involving the X. Here, we test the unguarded X hypothesis by forcing D. melanogaster females from a laboratory population to express recessive X-linked alleles to the same degree as males, using females exclusively made homozygous for the X chromosome. We find no evidence for reduced life span or egg-to-adult viability due to X homozygozity. In contrast, males and females homozygous for an autosome both suffer similar, significant reductions in those traits. The logic of the unguarded X hypothesis is indisputable, but our results suggest that the degree to which recessive deleterious X-linked alleles depress performance in the heterogametic sex appears too small to explain general sex differences in life span.

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