4.6 Article

Pro-autophagic polyphenols reduce the acetylation of cytoplasmic proteins

期刊

CELL CYCLE
卷 11, 期 20, 页码 3851-3860

出版社

LANDES BIOSCIENCE
DOI: 10.4161/cc.22027

关键词

Beclin 1; LC3; longevity; p62/SQSTM1; trichostatin A; U2OS

资金

  1. Ligue Nationale contre le Cancer (LNC, Equipe labelisee)
  2. Agence Nationale pour la Recherche (ANR)
  3. European Commission (Active p53, Apo-Sys, ChemoRes, ApopTrain)
  4. Fondation pour la Recherche Medicale (FRM)
  5. Institut National du Cancer (INCa)
  6. Canceropole Ile-de-France
  7. Fondation Bettencourt-Schueller
  8. LabEx Immuno-Oncology
  9. EMBO fellowship
  10. Junta de Extremadura
  11. Higher Education Commission (HEC) of Pakistan

向作者/读者索取更多资源

Resveratrol is a polyphenol contained in red wine that has been amply investigated for its beneficial effects on organismal metabolism, in particular in the context of the so-called French paradox, i.e., the relatively low incidence of coronary heart disease exhibited by a population with a high dietary intake of cholesterol and saturated fats. At least part of the beneficial effect of resveratrol on human health stems from its capacity to promote autophagy by activating the NAD-dependent deacetylase sirtuin 1. However, the concentration of resveratrol found in red wine is excessively low to account alone for the French paradox. Here, we investigated the possibility that other mono- and polyphenols contained in red wine might induce autophagy while affecting the acetylation levels of cellular proteins. Phenolic compounds found in red wine, including anthocyanins (oenin), stilbenoids (piceatannol), monophenols (caffeic acid, gallic acid) glucosides (delphinidin, kuronamin, peonidin) and flavonoids (catechin, epicatechin, quercetin, myricetin), were all capable of stimulating autophagy, although with dissimilar potencies. Importantly, a robust negative correlation could be established between autophagy induction and the acetylation levels of cytoplasmic proteins, as determined by a novel immunofluorescence staining protocol that allows for the exclusion of nuclear components from the analysis. Inhibition of sirtuin 1 by both pharmacological and genetic means abolished protein deacetylation and autophagy as stimulated by resveratrol, but not by piceatannol, indicating that these compounds act through distinct molecular pathways. In support of this notion, resveratrol and piceatannol synergized in inducing autophagy as well as in promoting cytoplasmic protein deacetylation. Our results highlight a cause-effect relationship between the deacetylation of cytoplasmic proteins and autophagy induction by red wine components.

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