Literature DB >> 23283301

A novel AMPK-dependent FoxO3A-SIRT3 intramitochondrial complex sensing glucose levels.

Alessia Peserico1, Fulvio Chiacchiera, Valentina Grossi, Antonio Matrone, Dominga Latorre, Marta Simonatto, Aurora Fusella, James G Ryall, Lydia W S Finley, Marcia C Haigis, Gaetano Villani, Pier Lorenzo Puri, Vittorio Sartorelli, Cristiano Simone.   

Abstract

Reduction of nutrient intake without malnutrition positively influences lifespan and healthspan from yeast to mice and exerts some beneficial effects also in humans. The AMPK-FoxO axis is one of the evolutionarily conserved nutrient-sensing pathways, and the FOXO3A locus is associated with human longevity. Interestingly, FoxO3A has been reported to be also a mitochondrial protein in mammalian cells and tissues. Here we report that glucose restriction triggers FoxO3A accumulation into mitochondria of fibroblasts and skeletal myotubes in an AMPK-dependent manner. A low-glucose regimen induces the formation of a protein complex containing FoxO3A, SIRT3, and mitochondrial RNA polymerase (mtRNAPol) at mitochondrial DNA-regulatory regions causing activation of the mitochondrial genome and a subsequent increase in mitochondrial respiration. Consistently, mitochondrial transcription increases in skeletal muscle of fasted mice, with a mitochondrial DNA-bound FoxO3A/SIRT3/mtRNAPol complex detectable also in vivo. Our results unveil a mitochondrial arm of the AMPK-FoxO3A axis acting as a recovery mechanism to sustain energy metabolism upon nutrient restriction.

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Year:  2013        PMID: 23283301     DOI: 10.1007/s00018-012-1244-6

Source DB:  PubMed          Journal:  Cell Mol Life Sci        ISSN: 1420-682X            Impact factor:   9.261


  41 in total

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3.  Glucose restriction can extend normal cell lifespan and impair precancerous cell growth through epigenetic control of hTERT and p16 expression.

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5.  Stress-dependent regulation of FOXO transcription factors by the SIRT1 deacetylase.

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6.  p38alpha blockade inhibits colorectal cancer growth in vivo by inducing a switch from HIF1alpha- to FoxO-dependent transcription.

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  38 in total

Review 1.  FoxO transcription factors: their roles in the maintenance of skeletal muscle homeostasis.

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Review 3.  Sirtuins and the Metabolic Hurdles in Cancer.

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Review 4.  Using mitochondrial sirtuins as drug targets: disease implications and available compounds.

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6.  Sirtuin 3 mediates neuroprotection of ketones against ischemic stroke.

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7.  SirT3 regulates the mitochondrial unfolded protein response.

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Review 8.  SIRT3: as simple as it seems?

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Review 9.  Mitochondrial Sirtuins and Molecular Mechanisms of Aging.

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Review 10.  Stem cell aging: mechanisms, regulators and therapeutic opportunities.

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