| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 10815855 | Cellular Signalling | 2016 | 32 Pages |
Abstract
AMP-activated protein kinase (AMPK) and its yeast homolog, Snf1, are critical regulators in the maintenance of energy metabolic balance not only stimulating energy production but also inhibiting energy-consuming processes. The AMPK/Snf1 signaling controls energy metabolism by specific phosphorylation of many metabolic enzymes and transcription factors, enhancing or suppressing their functions. The AMPK/Snf1 complexes can be translocated from cytoplasm into nuclei where they are involved in the regulation of transcription. Recent studies have indicated that AMPK/Snf1 activation can control histone acetylation through different mechanisms affecting not only gene transcription but also many other epigenetic functions. For instance, AMPK/Snf1 enzymes can phosphorylate the histone H3S10 (yeast) and H2BS36 (mammalian) sites which activate specific histone acetyltransferases (HAT), consequently enhancing histone acetylation. Moreover, nuclear AMPK can phosphorylate type 2A histone deacetylases (HDAC), e.g. HDAC4 and HDAC5, triggering their export from nuclei thus promoting histone acetylation reactions. AMPK activation can also increase the level of acetyl CoA, e.g. by inhibiting fatty acid and cholesterol syntheses. Acetyl CoA is a substrate for HATs, thus increasing their capacity for histone acetylation. On the other hand, AMPK can stimulate the activity of nicotinamide phosphoribosyltransferase (NAMPT) which increases the level of NAD+. NAD+ is a substrate for nuclear sirtuins, especially for SIRT1 and SIRT6, which deacetylate histones and transcription factors, e.g. those regulating ribosome synthesis and circadian clocks. Histone acetylation is an important epigenetic modification which subsequently can affect chromatin remodeling, e.g. via bromodomain proteins. We will review the signaling mechanisms of AMPK/Snf1 in the control of histone acetylation and subsequently clarify their role in the epigenetic regulation of ribosome synthesis and circadian clocks.
Keywords
Smad3MLL1PDHTAK1LSD1E1ADnmt1Sir2httERCTIF-IANLSHMG-CoANAMPTACAT1SCNPGC-1αSnRK1KDM2Ahistone 2Bperoxisome proliferator-activated receptor γ coactivator-1αrRNADBC1H2BSuv39h1SNF1GLUT4NMLINO1BRD4CaMKKβDNA methyltransferase 15-aminoimidazole-4-carboxamide ribonucleosideCryptochromeMEF2hsp70HDACacetoacetyl-CoA thiolaseCOAmTORGAPDHHMGRSIRTRDNAHIF-1αnESAICARACCNF-κBPPAR-γLKB1CREBAMPK3-hydroxy-3-methylglutaryl coenzyme AAMP-activated protein kinaseBmal1Ribosomal DNAHMG-CoA reductasePer2Ribosomal RNARNA polymerase Iacetyl-CoA carboxylaseAcetyl CoAHistone acetylationEpigeneticsilent information regulatorsilent information regulator 2sagaClockAgingnuclear localization signalBETmyocyte enhancer factor-2hypoxia-inducible factor-1αnuclear factor-κBFoxOATACSmileGlucose transporter type 4nicotinamide phosphoribosyltransferaseHuntingtinmammalian target of rapamycinSuprachiasmatic nucleiHistone acetyltransferasehistone deacetylasecyclic AMP response element binding proteinheat-shock protein 70Pol Ipyruvate dehydrogenasecasein kinase 1ChromatinHATcoenzyme Aliver kinase B1Cryglyceraldehyde 3-phosphate dehydrogenasePeroxisome proliferator-activated receptor-γ
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Authors
Antero Salminen, Anu Kauppinen, Kai Kaarniranta,