Genome-wide analysis in Drosophila reveals age-specific effects of SNPs on fitness traits
Genome-wide analysis in Drosophila reveals age-specific effects of SNPs on fitness traits
Most organisms exhibit senescence; a decline in physiological function with age. In nature, rates of senescence vary extensively among individuals and this variation has a significant genetic component; however, we know little about the genes underlying senescence. Here we show the first evidence that individual alleles influence fecundity in an age-specific manner and so the genetic basis of natural variation in fecundity changes dramatically with age. We complete a genome-wide association to identify single-nucleotide polymorphisms (SNPs) affecting lifespan and age-specific fecundity using the Drosophila melanogaster Genetic Reference Panel. We identify 1,031 SNPs affecting fecundity and 52 influencing lifespan. Only one SNP is associated with both early- and late-age fecundity. The age-specific effect of candidate genes on fecundity is validated using RNA interference. In addition, there is a dramatic increase in the number of SNPs influencing fecundity with age. This result provides support for the mutation accumulation theory of aging.
- University System of Maryland at Hagerstown United States
- Australian National University Australia
- North Carolina Agricultural and Technical State University United States
- North Carolina State University United States
- University of Maryland, Baltimore United States
Male, Aging, senescence, fertilit, fecundity, 590, Quantitative trait, Polymorphism, Single Nucleotide, single-nucleotide polymorphisms (SNPs), polymorphism, Animals, controlled study, Genetic variation, genome, transcription factor, aging, allele, article, transfer RNA, fitness, fly, Ageing, female, Drosophila melanogaster, Fertility, Gene Ontology, Keywords: immunoglobulin, genetic variation, Mutation, Female, Genetic Fitness, mutation, physiological response, Genome-Wide Association Study
Male, Aging, senescence, fertilit, fecundity, 590, Quantitative trait, Polymorphism, Single Nucleotide, single-nucleotide polymorphisms (SNPs), polymorphism, Animals, controlled study, Genetic variation, genome, transcription factor, aging, allele, article, transfer RNA, fitness, fly, Ageing, female, Drosophila melanogaster, Fertility, Gene Ontology, Keywords: immunoglobulin, genetic variation, Mutation, Female, Genetic Fitness, mutation, physiological response, Genome-Wide Association Study
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