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Identification of evolutionarily conserved genetic regulators of cellular aging
Authors:Laschober Gerhard T  Ruli Doris  Hofer Edith  Muck Christoph  Carmona-Gutierrez Didac  Ring Julia  Hutter Eveline  Ruckenstuhl Christoph  Micutkova Lucia  Brunauer Regina  Jamnig Angelika  Trimmel Daniela  Herndler-Brandstetter Dietmar  Brunner Stefan  Zenzmaier Christoph  Sampson Natalie  Breitenbach Michael  Fröhlich Kai-Uwe  Grubeck-Loebenstein Beatrix  Berger Peter  Wieser Matthias  Grillari-Voglauer Regina  Thallinger Gerhard G  Grillari Johannes  Trajanoski Zlatko  Madeo Frank  Lepperdinger Günter  Jansen-Dürr Pidder
Institution:Institute for Biomedical Aging Research, Austrian Academy of Sciences, Rennweg 10, A-6020 Innsbruck, Austria.
Abstract:To identify new genetic regulators of cellular aging and senescence, we performed genome-wide comparative RNA profiling with selected human cellular model systems, reflecting replicative senescence, stress-induced premature senescence, and distinct other forms of cellular aging. Gene expression profiles were measured, analyzed, and entered into a newly generated database referred to as the GiSAO database. Bioinformatic analysis revealed a set of new candidate genes, conserved across the majority of the cellular aging models, which were so far not associated with cellular aging, and highlighted several new pathways that potentially play a role in cellular aging. Several candidate genes obtained through this analysis have been confirmed by functional experiments, thereby validating the experimental approach. The effect of genetic deletion on chronological lifespan in yeast was assessed for 93 genes where (i) functional homologues were found in the yeast genome and (ii) the deletion strain was viable. We identified several genes whose deletion led to significant changes of chronological lifespan in yeast, featuring both lifespan shortening and lifespan extension. In conclusion, an unbiased screen across species uncovered several so far unrecognized molecular pathways for cellular aging that are conserved in evolution.
Keywords:aging  evolution  replicative lifespan  replicative senescence  senescence  yeast
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