Acetylation of p53 Is Involved in Valproic Acid Induced Death of AML Cells

Thakur, Binay; Dittrich, Tino; Welte, Karl; Klusmann, Jan‐Henning; Reinhardt, Dirk

doi:10.1182/blood.v118.21.2461.2461

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“…From a mechanistic viewpoint there may also be a number of different pathways through which HDACi treatment results in this increased expression of p21. This includes the elevated acetylation of p53, which has been observed following treatment with tributyrin ( de Conti et al, 2013 ; Ortega et al, 2016 ), sodium butyrate ( Terui et al, 2003 ; Ortega et al, 2016 ), romidepsin ( Zhao et al, 2006 ), VPA ( Thakur et al, 2011 ), vorinistat ( Seo et al, 2011 ; Nebbioso et al, 2017 ), and entinostat ( Miller et al, 2011 ). As an important tumor suppressor, and key transcriptional activator of p21, the increased acetylation of p53 is quite likely to be involved in the response to HDACi in neuroblastoma.…”

Section: Hdac Inhibitors In Neuroblastomamentioning

confidence: 99%

Histone Deacetylases and Histone Deacetylase Inhibitors in Neuroblastoma

Phimmachanh

Han

O'Donnell

et al. 2020

Front. Cell Dev. Biol.

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Histone deacetylases (HDACs) are enzymes that play a key role in regulating gene expression by remodeling chromatin structure. An imbalance of histone acetylation caused by deregulated HDAC expression and activity is known to promote tumor progression in a number of tumor types, including neuroblastoma, the most common solid tumor in children. Consequently, the inhibition of HDACs has emerged as a potential strategy to reverse these aberrant epigenetic changes, and several classes of HDAC inhibitors (HDACi) have been shown to inhibit tumor proliferation, or induce differentiation, apoptosis and cell cycle arrest in neuroblastoma. Further, the combined use of HDACi with other chemotherapy agents, or radiotherapy, has shown promising pre-clinical results and various HDACi have progressed to different stages in clinical trials. Despite this, the effects of HDACi are multifaceted and more work needs to be done to unravel their specific mechanisms of actions. In this review, we discuss the functional role of HDACs in neuroblastoma and the potential of HDACi to be optimized for development and use in the clinic for treatment of patients with neuroblastoma.

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