Lifespan changes: From wild type to ctl-1;ctl-2;ctl-3;sod-1
20
24.3
Quadruple mutant ctl-1(wuIs151);ctl-2(wuIs151);ctl-3(wuIs151);sod-1(wuIs152) has a lifespan of 24.3 days, while single mutant sod-1(wuIs152) has a lifespan of 25.6 days and triple mutant ctl-1(wuIs151);ctl-2(wuIs151);ctl-3(wuIs151) has a lifespan of 16.1 days.
Cabreiro F et al., 2011, Increased life span from overexpression of superoxide dismutase in Caenorhabditis elegans is not caused by decreased oxidative damage. Free Radic Biol Med. 51(8):1575-82 21839827 Click here to select all mutants from this PubMed ID in the graph
20
20.0
Quadruple mutant ctl-1(wuIs151);ctl-2(wuIs151);ctl-3(wuIs151);sod-1(wuIs154) has a lifespan of 20.0 days, while single mutant sod-1(wuIs154) has a lifespan of 21.5 days and triple mutant ctl-1(wuIs151);ctl-2(wuIs151);ctl-3(wuIs151) has a lifespan of 16.1 days.
Cabreiro F et al., 2011, Increased life span from overexpression of superoxide dismutase in Caenorhabditis elegans is not caused by decreased oxidative damage. Free Radic Biol Med. 51(8):1575-82 21839827 Click here to select all mutants from this PubMed ID in the graph
Catalase-2
Locus: CELE_Y54G11A.6
Wormbase description: ctl-1 encodes one of three C. elegans catalases; CTL-1 exhibits catalase activity in vitro, and thus likely functions in vivo as an antioxidant enzyme that protects cells from reactive oxygen species; ctl-1 activity contributes to the extended lifespan seen in daf-2 mutant animals; in addition, ctl-1 expression is negatively regulated by DAF-2-mediated insulin signaling; as CTL-1 does not possess a C-terminal peroxisomal targeting signal (PTS), it is predicted to be a cytosolic catalase.
Peroxisomal catalase 1
Locus: CELE_Y54G11A.5
Wormbase description: ctl-2 encodes one of three C. elegans catalases; CTL-2 exhibits catalase and peroxidase activity in vitro, and thus likely functions in vivo as an antioxidant enzyme that protects cells from reactive oxygen species; ctl-2 activity is required for normal lifespan as well as for the extended lifespan seen in daf-2 mutant animals; in addition, ctl-2 is required for normal egg-laying capacity and for normal peroxisomal morphology; immunoelectron microscopy indicates that CTL-2 is found mainly in the peroxisomes of intestinal epithelial cells; ctl-2 expression is negatively regulated by DAF-2-mediated insulin signaling.
Catalase
Locus: CELE_Y54G11A.13
Wormbase description: ctl-3 encodes one of three C. elegans catalases; CTL-3 is predicted to function as an antioxidant enzyme that protects cells from reactive oxygen species; a ctl-3 promoter gfp fusion construct is expressed in pharyngeal muscles and neuronal cell bodies; loss of ctl-3 activity via RNAi results in no obvious abnormalities.
Superoxide dismutase [Cu-Zn]
Locus: CELE_C15F1.7
Wormbase description: sod-1 encodes the copper/zinc superoxide dismustase, an enzyme that is known to protect cells from oxidative damage; superoxide dismutase activity can be detected in worm extracts; sod-1 activity has been implicated in the increased life-span of dauer larvae where this enzyme demonstrates the highest activity compared to other life-stages as well as in the increased life span of age-1 mutants and their resistance to oxidative damage; sod-1 modulates the effect of let-60 ras on vulval and germline development via cytoplasmic reactive oxygen species; unlike other eukaryotic superoxide dismutases, sod-1 does not require the copper chaperone CCS for its activity and instead uses a glutathione pathway for acquiring copper; in humans, mutation of SOD1 (OMIM:147450) leads to amyotrophic lateral sclerosis (OMIM:105400).
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SynergyAge database hosts high-quality, manually curated information about the synergistic and antagonistic lifespan effects of genetic interventions in model organisms, also allowing users to explore the longevity relationships between genes in a visual way.
If you would like to cite this database please use:
Bunu, G., Toren, D., Ion, C. et al. SynergyAge, a curated database for synergistic and antagonistic interactions of longevity-associated genes. Sci Data 7, 366 (2020). https://doi.org/10.1038/s41597-020-00710-z
Group webpage: www.aging-research.group