Age-Specific Variation in Immune Response in Drosophila melanogaster Has a Genetic Basis

dc.contributor.authorFelix, Tashauna M
dc.contributor.authorHughes, Kimberly A
dc.contributor.authorStone, Eric A
dc.contributor.authorDrnevich,  Jenny M
dc.contributor.authorLeips, Jeff
dc.date.accessioned2023-08-07T20:43:00Z
dc.date.available2023-08-07T20:43:00Z
dc.date.issued2012-07-01
dc.description.abstractImmunosenescence, the age-related decline in immune system function, is a general hallmark of aging. While much is known about the cellular and physiological changes that accompany immunosenescence, we know little about the genetic influences on this phenomenon. In this study we combined age-specific measurements of bacterial clearance ability following infection with whole-genome measurements of the transcriptional response to infection and wounding to identify genes that contribute to the natural variation in immunosenescence, using Drosophila melanogaster as a model system. Twenty inbred lines derived from nature were measured for their ability to clear an Escherichia coli infection at 1 and 4 weeks of age. We used microarrays to simultaneously determine genome-wide expression profiles in infected and wounded flies at each age for 12 of these lines. Lines exhibited significant genetically based variation in bacterial clearance at both ages; however, the genetic basis of this variation changed dramatically with age. Variation in gene expression was significantly correlated with bacterial clearance ability only in the older age group. At 4 weeks of age variation in the expression of 247 genes following infection was associated with genetic variation in bacterial clearance. Functional annotation analyses implicate genes involved in energy metabolism including those in the insulin signaling/TOR pathway as having significant associations with bacterial clearance in older individuals. Given the evolutionary conservation of the genes involved in energy metabolism, our results could have important implications for understanding immunosenescence in other organisms, including humans.en
dc.description.sponsorshipWe thank Maria De Luca, Michelle Starz-Gaiano, Maricel Kann, and Joseph Travis for insightful discussion of the results. Michelle Starz-Gaiano and Maria De Luca provided helpful comments on the manuscript. We thank Tim Ford for formatting the figures. T.M.F. was supported by U.S. Department of Education award P200A060197, National Institute of General Medical Sciences Initiative for Maximizing Student Development grant R25-GM55036, and Procter and Gamble. K.A.H. was supported by National Science Foundation grant DEB 0848337. This research was supported by National Institutes of Health grants 1R03 AG023339-01 and 5R01 DK084219-02 (to J.L.).en
dc.description.urihttps://academic.oup.com/genetics/article/191/3/989/5935010en
dc.genrejournal articlesen
dc.identifierdoi:10.13016/m2q6bb-qgw8
dc.identifier.citationTashauna M Felix and others, Age-Specific Variation in Immune Response in Drosophila melanogaster Has a Genetic Basis, Genetics, Volume 191, Issue 3, 1 July 2012, Pages 989–1002, https://doi.org/10.1534/genetics.112.140640en
dc.identifier.urihttps://doi.org/10.1534/genetics.112.140640
dc.identifier.urihttp://hdl.handle.net/11603/29110
dc.language.isoenen
dc.publisherOxford University Pressen
dc.relation.isAvailableAtThe University of Maryland, Baltimore County (UMBC)
dc.relation.ispartofUMBC Biological Sciences Department Collection
dc.relation.ispartofUMBC Faculty Collection
dc.relation.ispartofUMBC Student Collection
dc.rightsThis item is likely protected under Title 17 of the U.S. Copyright Law. Unless on a Creative Commons license, for uses protected by Copyright Law, contact the copyright holder or the author.en
dc.subjectgenetic variationen
dc.subjectbacterial clearanceen
dc.subjectwound responseen
dc.subjectagingen
dc.subjectimmunosenescenceen
dc.titleAge-Specific Variation in Immune Response in Drosophila melanogaster Has a Genetic Basisen
dc.typeTexten
dcterms.creatorhttps://orcid.org/0000-0001-8999-6630en

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