Tor‐Sch9 deficiency activates catabolism of the ketone body‐like acetic acid to promote trehalose accumulation and longevity |
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| Authors: | Jia Hu Min Wei Hamed Mirzaei Federica Madia Mario Mirisola Camille Amparo Shawna Chagoury Brian Kennedy Valter D Longo |
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| Institution: | 1. Longevity Institute, Davis School of Gerontology, University of Southern California, , Los Angeles, CA, 90089 USA;2. Department of Biological Sciences, School of Dornsife College of Letters, Arts and Sciences, University of Southern California, , Los Angeles, CA, 90089 USA;3. DiBiMeF, Universita’ di Palermo, , 90133 Palermo, Italy;4. Buck Institute for Research on Aging, , Novato, CA, 94945 USA |
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| Abstract: | In mammals, extended periods of fasting leads to the accumulation of blood ketone bodies including acetoacetate. Here we show that similar to the conversion of leucine to acetoacetate in fasting mammals, starvation conditions induced ketone body‐like acetic acid generation from leucine in S. cerevisiae. Whereas wild‐type and ras2Δ cells accumulated acetic acid, long‐lived tor1Δ and sch9Δ mutants rapidly depleted it through a mitochondrial acetate CoA transferase‐dependent mechanism, which was essential for lifespan extension. The sch9Δ‐dependent utilization of acetic acid also required coenzyme Q biosynthetic genes and promoted the accumulation of intracellular trehalose. These results indicate that Tor‐Sch9 deficiency extends longevity by switching cells to an alternative metabolic mode, in which acetic acid can be utilized for the storage of stress resistance carbon sources. These effects are reminiscent of those described for ketone bodies in fasting mammals and raise the possibility that the lifespan extension caused by Tor‐S6K inhibition may also involve analogous metabolic changes in higher eukaryotes. |
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| Keywords: | acetic acid aging chronological lifespan leucine Sch9 |
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