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Loss of Nat4 and its associated histone H4 N-terminal acetylation mediates calorie restriction-induced longevity
D. Molina-Serrano, V. Schiza, C. Demosthenous, E. Stavrou, J. Oppelt, D. Kyriakou, W. Liu, G. Zisser, H. Bergler, W. Dang, A. Kirmizis,
Language English Country England, Great Britain
Document type Journal Article
NLK
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Nature Open Access
from 2014-04-01
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- MeSH
- Acetylation MeSH
- Transcriptional Activation MeSH
- Time Factors MeSH
- Chromatin metabolism MeSH
- Longevity MeSH
- Down-Regulation MeSH
- Histone Acetyltransferases metabolism MeSH
- Histones metabolism MeSH
- Caloric Restriction * MeSH
- N-Terminal Acetyltransferase D deficiency genetics physiology MeSH
- Nicotinamidase genetics metabolism MeSH
- Protein Processing, Post-Translational MeSH
- Gene Expression Regulation, Fungal * MeSH
- Saccharomyces cerevisiae Proteins genetics metabolism physiology MeSH
- Saccharomyces cerevisiae genetics physiology MeSH
- Gene Expression Profiling MeSH
- Publication type
- Journal Article MeSH
Changes in histone modifications are an attractive model through which environmental signals, such as diet, could be integrated in the cell for regulating its lifespan. However, evidence linking dietary interventions with specific alterations in histone modifications that subsequently affect lifespan remains elusive. We show here that deletion of histone N-alpha-terminal acetyltransferase Nat4 and loss of its associated H4 N-terminal acetylation (N-acH4) extend yeast replicative lifespan. Notably, nat4Δ-induced longevity is epistatic to the effects of calorie restriction (CR). Consistent with this, (i) Nat4 expression is downregulated and the levels of N-acH4 within chromatin are reduced upon CR, (ii) constitutive expression of Nat4 and maintenance of N-acH4 levels reduces the extension of lifespan mediated by CR, and (iii) transcriptome analysis indicates that nat4Δ largely mimics the effects of CR, especially in the induction of stress-response genes. We further show that nicotinamidase Pnc1, which is typically upregulated under CR, is required for nat4Δ-mediated longevity. Collectively, these findings establish histone N-acH4 as a regulator of cellular lifespan that links CR to increased stress resistance and longevity.
Department of Biological Sciences University of Cyprus Nicosia Cyprus
Huffington Center on Aging Baylor College of Medicine Houston TX USA
Institut für Molekulare Biowissenschaften Karl Franzens Universität Graz Austria
References provided by Crossref.org
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