DNA damage activates p53 through a phosphorylation–acetylation cascade

Sakaguchi, Kazuyasu; Herrera, Julio E.; Saito, Shinichi; Miki, Toru; Bustin, Michael; Vassilev, Alex; Anderson, Carl W.; Appella, Ettore

doi:10.1101/gad.12.18.2831

Cited by 1,101 publications

(1,193 citation statements)

References 47 publications

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“…Several studies have shown the apoptotic role of p53 acetylation at the K320 residue (Sakaguchi et al ., 1998; Terui et al ., 2003; Roy et al ., 2005; Brandl et al ., 2012). In order to determine whether SIRT3 modulates p53 acetylation, we performed Western blot analysis after cotransfection of SIRT3 and p53 constructs in SH‐SY5Y cells.…”

Section: Resultsmentioning

confidence: 99%

“…In addition, SIRT3 overexpression nullified the pathological changes induced by WT p53 and p53 K320Q, supporting our hypothesis that SIRT3 prevents p53‐induced mitochondrial dysfunction and neuronal cell death. Previous studies support our finding that p53 acetylation at the K320 residue is linked to cell damage (Sakaguchi et al ., 1998; Terui et al ., 2003; Roy et al ., 2005; Brandl et al ., 2012). Importantly, we found that Ac‐p53 K320 levels are significantly increased in the mitochondria of AD in conjunction with reduced SIRT3 levels.…”

Section: Discussionmentioning

confidence: 99%

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SIRT3 deregulation is linked to mitochondrial dysfunction in Alzheimer's disease

et al. 2017

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SummaryAlzheimer's disease (AD) is the leading cause of dementia in the elderly. Despite decades of study, effective treatments for AD are lacking. Mitochondrial dysfunction has been closely linked to the pathogenesis of AD, but the relationship between mitochondrial pathology and neuronal damage is poorly understood. Sirtuins (SIRT, silent mating type information regulation 2 homolog in yeast) are NAD‐dependent histone deacetylases involved in aging and longevity. The objective of this study was to investigate the relationship between SIRT3 and mitochondrial function and neuronal activity in AD. SIRT3 mRNA and protein levels were significantly decreased in AD cerebral cortex, and Ac‐p53 K320 was significantly increased in AD mitochondria. SIRT3 prevented p53‐induced mitochondrial dysfunction and neuronal damage in a deacetylase activity‐dependent manner. Notably, mitochondrially targeted p53 (mito‐p53) directly reduced mitochondria DNA‐encoded ND2 and ND4 gene expression resulting in increased reactive oxygen species (ROS) and reduced mitochondrial oxygen consumption. ND2 and ND4 gene expressions were significantly decreased in patients with AD. p53‐ChIP analysis verified the presence of p53‐binding elements in the human mitochondrial genome and increased p53 occupancy of mitochondrial DNA in AD. SIRT3 overexpression restored the expression of ND2 and ND4 and improved mitochondrial oxygen consumption by repressing mito‐p53 activity. Our results indicate that SIRT3 dysfunction leads to p53‐mediated mitochondrial and neuronal damage in AD. Therapeutic modulation of SIRT3 activity may ameliorate mitochondrial pathology and neurodegeneration in AD.

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Section: Resultsmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

SIRT3 deregulation is linked to mitochondrial dysfunction in Alzheimer's disease

et al. 2017

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“…The parental HCT116 cells express a protein truncated downstream of the HAT domain (hence only detectable with the N-terminal antibody), which has been shown to be functionally normal (Sakaguchi et al, 1998;Sun et al, 2000;Iyer et al, 2004a). We have previously shown that the single HCT116 allele that is expressed was disrupted by homologous recombination, generating a p300 null cell line (p300 À ).…”

Section: Resultsmentioning

confidence: 99%

p300 is required for orderly G1/S transition in human cancer cells

Jian

Chin

et al. 2006

Oncogene

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“…Phosphorylation of human P53 at serine 392 and/or acetylation at lysine 382 occur after DNA damage (Hao et al, 1996;Lu et al, 1997;Sakaguchi et al, 1998). Silencing of BRG1 induced strong P53 activation, as observed in its phosphorylated and acetylated forms (Figure 7b).…”

Section: Genes Involved In Dna Repairmentioning

confidence: 89%

The BRG1 ATPase of chromatin remodeling complexes is involved in modulation of mesenchymal stem cell senescence through RB–P53 pathways

et al. 2010

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We focused our attention on brahma-related gene 1 (BRG1), the ATPase subunit of the SWItch/Sucrose NonFermentable (SWI/SNF) chromatin remodeling complex, and analyzed its role in mesenchymal stem cell (MSC) biology. We hypothesized that deviation from the correct concentration of these proteins, which act at the highest level of gene regulation, may be deleterious for cells. We wanted to know what would happen if a cell had to cope with altered regulation of gene expression, either by upregulation or downregulation of BRG1. We assumed that cells would try to restore homeostasis or, alternatively, that the event could trigger senescence/apoptosis phenomena. To this end, in MSCs, we silenced BRG1gene. Knockdown of BRG1 expression induced a significant increase in senescent cells and decrease in apoptotic cells. It is interesting that BRG1 downregulation also induced an increase in heterochromatin. At the molecular level, these phenomena were associated with activation of retinoblastoma-like protein 2 (RB2)/P130-and P53-related pathways. Senescence was accompanied by reduced expression of some stemness-related genes. This is consistent with our previous research, which showed that BRG1 upregulation by ectopic expression also induced senescence processes. Together, these data suggest that BRG1 belongs to a class of genes whose expression is tightly regulated; hence, subtle alterations in BRG1 activity seem to negatively affect mechanisms regulating chromatin status and, in turn, impair cellular physiology.

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DNA damage activates p53 through a phosphorylation–acetylation cascade

Cited by 1,101 publications

References 47 publications

SIRT3 deregulation is linked to mitochondrial dysfunction in Alzheimer's disease

SIRT3 deregulation is linked to mitochondrial dysfunction in Alzheimer's disease

p300 is required for orderly G1/S transition in human cancer cells

The BRG1 ATPase of chromatin remodeling complexes is involved in modulation of mesenchymal stem cell senescence through RB–P53 pathways

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