[No authors listed]
In an initial preliminary screen we identified factors associated with controlling Drosophila aging by examining longevity in adults where EP elements induced over-expression or antisense-RNA at genes adjacent to each insertion. Here, we study 45 EP lines that initially showed at least 10% longer mean lifespan than controls. These 45 lines and a daughterless (da)-Gal4 stock were isogenized into a CS10 wild-type background. Sixteen EP lines corresponding to 15 genes significantly extended lifespan when their target genes were driven by da-Gal4. In each case, the target genes were seen to be over-expressed. Independently derived UAS-gene transgenic stocks were available or made for two candidates: ImpL2 which is ecdysone-inducible gene L2, and CG33138, 1,4-alpha-glucan branching enzyme. With both, adult lifespan was increased upon over-expression via the GeneSwitch inducible Gal4 driver system. Several genes in this set of 15 correspond to previously discovered longevity assurance systems such as insulin/IGF-1 signaling, gene silencing, and autophagy; others suggest new potential mechanisms for the control of aging including mRNA synthesis and maturation, intracellular vesicle trafficking, and neuroendocrine regulation.
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CG42753, AGBE, kis, Thor, Rat1, RapGAP1, CG4901, CG5861, Lrch, CG10383, CG10338, vimar, Drip, Sin3A, Amph, nemy, GLS, CG42663, mam, CG10209, CG8155, Arf51F, CG10916, hts, CalpA, sm, CG3927, fabp, Hsromega, CG30427, CG13890, ImpL2, CG14997, eco, PGRP-LC, PGRP-LF, CG42268, RpL13A, Dlc90F, SIFaR, CG5807, CycB3, dan, CycG, gom, cv-2, Gug, Men, l(3)05822, Atpalpha, Mbs
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