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Wei M, et al.  (2009) Tor1/Sch9-regulated carbon source substitution is as effective as calorie restriction in life span extension. PLoS Genet 5(5):e1000467

Abstract: The effect of calorie restriction (CR) on life span extension, demonstrated in organisms ranging from yeast to mice, may involve the down-regulation of pathways, including Tor, Akt, and Ras. Here, we present data suggesting that yeast Tor1 and Sch9 (a homolog of the mammalian kinases Akt and S6K) is a central component of a network that controls a common set of genes implicated in a metabolic switch from the TCA cycle and respiration to glycolysis and glycerol biosynthesis. During chronological survival, mutants lacking SCH9 depleted extracellular ethanol and reduced stored lipids, but synthesized and released glycerol. Deletion of the glycerol biosynthesis genes GPD1, GPD2, or RHR2, among the most up-regulated in long-lived sch9Delta, tor1Delta, and ras2Delta mutants, was sufficient to reverse chronological life span extension in sch9Delta mutants, suggesting that glycerol production, in addition to the regulation of stress resistance systems, optimizes life span extension. Glycerol, unlike glucose or ethanol, did not adversely affect the life span extension induced by calorie restriction or starvation, suggesting that carbon source substitution may represent an alternative to calorie restriction as a strategy to delay aging.

Status: Published Type: Journal Article | Research Support, N.I.H., Extramural | Research Support, Non-U.S. Gov't PubMed ID: 19424415

Topics addressed in this paper

Number of different genes curated to this paper: 28

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Topics Topics not linked to Genes Genes linked to topics (#1 - 10 )
DAK1 DAK2 ERG28 ERG4 ERG5 FMP45 GCY1 GIS1 GPD1 GPD2
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Topics Genes linked to topics (#11 - 20 )
GRE1 HOR2 IME1 RAS1 RAS2 RHR2 RIM15 RPI1 SCH9 SPS100
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Topics Genes linked to topics (#21 - 28 )
TAH1 TCO89 TIS11 TOR1 YDL218W YIG1 YLR012C YPR1
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