Inhibition of SIRT1 Reactivates Silenced Cancer Genes without Loss of Promoter DNA Hypermethylation

Pruitt, Kevin; Zinn, Rebekah L.; Ohm, Joyce E.; McGarvey, Kelly M.; Kang, Sung Hae L.; Watkins, D. Neil; Herman, James G.; Baylin, Stephen B.

doi:10.1371/journal.pgen.0020040

Cited by 362 publications

(323 citation statements)

References 50 publications

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“…Interestingly, these two changes occurred only in the promoter region where SirT1 was localized. This observation agrees with many studies demonstrating that changes in histone acetylation levels that were associated with transcriptional regulation were often located exclusively in regulatory regions (CalestagneMorelli and Ausio´, 2006;Pruitt et al, 2006). Additionally, the finding that SirT1 also deacetylates H1K26Ac (Vaquero et al, 2004) might indicate that H1 recruitment and its deacetylation are coordinated and concomitant with heterochromatin formation.…”

Section: Sirt1supporting

confidence: 92%

“…SirT1 is present in cancer cells at the promoters of tumor suppressor genes, and its loss results in a hyperacetylation of H4K16 and H3K9 at these promoters; this in turn induces expression of these genes without affecting DNA hypermethylation (Pruitt et al, 2006). These observations confirm previous findings demonstrating that SirT1 targets H4K16Ac (Vaquero et al, 2004).…”

Section: Sirts Cancer and H4k16supporting

confidence: 90%

“…SirT1 is overexpressed in late stages of prostate cancer (Kuzmichev et al, 2005;Figure 4b) and in breast and colon cancers (Ashraf et al, 2006;Pruitt et al, 2006). SirT1 can deacetylate the tumor-suppressor p53 and this inhibits both p53 transcriptional activity and p53-dependent apoptosis upon cellular stress.…”

Section: Sirts Cancer and H4k16mentioning

confidence: 99%

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NAD+-dependent deacetylation of H4 lysine 16 by class III HDACs

2007

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Histone deacetylases (HDACs) catalyse the removal of acetyl groups from the N-terminal tails of histones. All known HDACs can be categorized into one of four classes (I-IV). The class III HDAC or silencing information regulator 2 (Sir2) family exhibits characteristics consistent with a distinctive role in regulation of chromatin structure. Accumulating data suggest that these deacetylases acquired new roles as genomic complexity increased, including deacetylation of non-histone proteins and functional diversification in mammals. However, the intrinsic regulation of chromatin structure in species as diverse as yeast and humans, underscores the pressure to conserve core functions of class III HDACs, which are also known as Sirtuins. One of the key factors that might have contributed to this preservation is the intimate relationship between some members of this group of proteins (SirT1, SirT2 and SirT3) and deacetylation of a specific residue in histone H4, lysine 16 (H4K16). Evidence accumulated over the years has uncovered a unique role for H4K16 in chromatin structure throughout eukaryotes. Here, we review the recent findings about the functional relationship between H4K16 and the Sir2 class of deacetylases and how that relationship might impact aging and diseases including cancer and diabetes.

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Section: Sirt1supporting

confidence: 92%

Section: Sirts Cancer and H4k16supporting

confidence: 90%

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NAD+-dependent deacetylation of H4 lysine 16 by class III HDACs

2007

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“…Whereas class I HDACs show little substrate specificity and the direct HDAC activity of class II HDACs has been debated, the class III HDAC SIRT1 has been reported to show preference for deacetylation of H4K16 (Vaquero et al, 2004(Vaquero et al, , 2007Pruitt et al, 2006). Further, HDACs 1-8 were ubiquitously expressed in H157 cells as assessed by immunoblotting, and did not show any change in expression after VPA or TSA exposure (data not shown).…”

Section: Sirt1 Inhibition Mediates Increase In H4k16 Acetylation and mentioning

confidence: 94%

Opposing effects of hMOF and SIRT1 on H4K16 acetylation and the sensitivity to the topoisomerase II inhibitor etoposide

Wallenborg

Vlachos

et al. 2010

Oncogene

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Various inhibitors of histone deacetylase (HDAC) activity can sensitize drug resistant cancer cells to chemotherapeutic agents. However, the mechanisms underlying such effects of distinct HDAC inhibitors (HDACi) remain poorly understood. Here we show that both the HDACi trichostatin A and valproic acid induced a sensitization of multidrug-resistant cancer cells to the topoisomerase II inhibitor etoposide/VP16. This effect was associated with increased acetylation of certain lysines on histones H3 and H4, including lysine 16 on histone H4 (H4K16). Overexpression of the histone acetyltransferase hMOF, known to target H4K16, was sufficient to mimic HDACi treatment on sensitization and H4K16 acetylation, and importantly, small-interfering RNA (siRNA)-mediated knockdown of hMOF abolished the HDACi-mediated sensitizing effects as well as the increase in H4K16 acetylation. Conversely, siRNA-mediated knockdown of the H4K16 deacetylase SIRT1 mimicked HDACi treatment whereas overexpression of SIRT1 abolished H4K16 acetylation and significantly reduced the sensitizing effects of HDACi. Interestingly, the effects of hMOF on H4K16 acetylation and sensitization to the topoisomerase II inhibitor could be directly counteracted by exogenous expression of increasing amounts of SIRT1 and vice versa. Our study results suggest that hMOF and SIRT1 activities are critical parameters in HDACi-mediated sensitization of multidrug-resistant cancer cells to topoisomerase II inhibitor and increased H4K16 acetylation.

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“…D'autre part, ces HAT avaient déjà été identifiées dans des réarrangements chromosomiques associés à des leucémies présentant une activité HAT K16 réduite [28]. À l'inverse de cette perte globale d'acétylation de K16, il a été montré que la ré-expression, au cours du processus tumoral, de gènes épigénétiquement réprimés coïncidait avec une augmentation de l'acétylation de K16 dans leurs régions promotrices bien que les marques épigénétiques de répression ne soient pas nécessairement éliminées [30,31]. C'est pourquoi la détection de variations globales d'acétylation de K16 serait un des marqueurs de développement de certains cancers et constituerait même un moyen de prédire l'évolution clinique du cancer (par exemple, le cancer de la prostate [29]).…”

Section: Lysine 16 Cancer Et Croissance Tumoraleunclassified

De la régulation du génome à la progression tumorale

Miotto

Struhl

2007

Med Sci (Paris)

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Inhibition of SIRT1 Reactivates Silenced Cancer Genes without Loss of Promoter DNA Hypermethylation

Cited by 362 publications

References 50 publications

NAD+-dependent deacetylation of H4 lysine 16 by class III HDACs

NAD+-dependent deacetylation of H4 lysine 16 by class III HDACs

Opposing effects of hMOF and SIRT1 on H4K16 acetylation and the sensitivity to the topoisomerase II inhibitor etoposide

De la régulation du génome à la progression tumorale

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