Drug-induced inactivation or gene silencing of class I histone deacetylases suppresses ovarian cancer cell growth: Implications for therapy

Khabele, Dineo; Son, Deok Soo; Parl, Angelika K.; Goldberg, Gary L.; Augenlicht, Leonard H.; Mariadason, John M.; Rice, Valerie Montgomery

doi:10.4161/cbt.6.5.4007

Cited by 97 publications

(113 citation statements)

References 29 publications

(48 reference statements)

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“…These findings are also consistent with the growth inhibitory effects of HDAC inhibitors on colon cancer cells (Archer et al, 1998;Wilson et al, 2006). Although it is known that class I HDACs are consistently up-regulated in human colon cancer and in other solid tumors at the mRNA and/or protein levels (Zhu et al, 2004;Huang et al, 2005;Wilson et al, 2006;Khabele et al, 2007), relatively less is known about HDAC4 expression in colon cancer. Although down-regulation of HDAC4 mRNA in human colon tumor tissue compared with normal has been shown (Lleonart et al, 2006), we detected no overall difference in HDAC4 protein expression between in a panel of matched human colon tumor-normal pairs (unpublished observations) in which clear overexpression of HDAC1, HDAC2, and HDAC3 was detected previously (Wilson et al, 2006).…”

supporting

confidence: 75%

“…A large body of literature indicates that HDAC inhibitors induce cell cycle arrest, differentiation, and apoptosis in colon cancer cell lines in vitro (Heerdt et al, 1994;Mariadason et al, 1997;Archer et al, 1998;Litvak et al, 1998;Mariadason et al, 2000Mariadason et al, , 2001bGurvich et al, 2004;Wilson et al, 2006). Based on such studies, several HDAC inhibitors, including depsipeptide, SAHA, MS-275, and valproic acid, are in clinical trials for the treatment of hemopoetic and solid tumors, including colon cancer (Mei et al, 2004;Bolden et al, 2006;Rasheed et al, 2007), with SAHA recently being approved for the treatment of patients with cutaneous T cell lymphoma.Several studies have demonstrated increased expression of the class I HDACs, HDAC1, HDAC2, and HDAC3, in multiple human cancers, including colon cancer (Zhu et al, 2004;Huang et al, 2005;Wilson et al, 2006;Khabele et al, 2007). Consistent with the ability of HDAC inhibitors to induce maturation in colon cancer cell lines, individual class I HDACs can repress p21 expression, promote cell proliferation and survival, and inhibit differentiation in vitro ( Wilson et al, 2006).…”

mentioning

confidence: 90%

“…Several studies have demonstrated increased expression of the class I HDACs, HDAC1, HDAC2, and HDAC3, in multiple human cancers, including colon cancer (Zhu et al, 2004;Huang et al, 2005;Wilson et al, 2006;Khabele et al, 2007). Consistent with the ability of HDAC inhibitors to induce maturation in colon cancer cell lines, individual class I HDACs can repress p21 expression, promote cell proliferation and survival, and inhibit differentiation in vitro (Lagger et al, 2002;Glaser et al, 2003;Zhu et al, 2004;Huang This article was published online ahead of print in MBC in Press (http://www.molbiolcell.org/cgi/doi/10.1091/mbc.E08 -02-0139) on July 16, 2008Wilson et al, 2006).…”

Section: Introductionmentioning

confidence: 99%

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HDAC4 Promotes Growth of Colon Cancer Cells via Repression of p21

Wilson

Byun

Nasser

et al. 2008

MBoC

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189

172

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The class II Histone deacetylase (HDAC), HDAC4, is expressed in a tissue-specific manner, and it represses differentiation of specific cell types. We demonstrate here that HDAC4 is expressed in the proliferative zone in small intestine and colon and that its expression is down-regulated during intestinal differentiation in vivo and in vitro. Subcellular localization studies demonstrated HDAC4 expression was predominantly nuclear in proliferating HCT116 cells and relocalized to the cytoplasm after cell cycle arrest. Down-regulating HDAC4 expression by small interfering RNA (siRNA) in HCT116 cells induced growth inhibition and apoptosis in vitro, reduced xenograft tumor growth, and increased p21 transcription. Conversely, overexpression of HDAC4 repressed p21 promoter activity. p21 was likely a direct target of HDAC4, because HDAC4 down-regulation increased p21 mRNA when protein synthesis was inhibited by cycloheximide. The importance of p21 repression in HDAC4-mediated growth promotion was demonstrated by the failure of HDAC4 down-regulation to induce growth arrest in HCT116 p21-null cells. HDAC4 down-regulation failed to induce p21 when Sp1 was functionally inhibited by mithramycin or siRNA-mediated down-regulation. HDAC4 expression overlapped with that of Sp1, and a physical interaction was demonstrated by coimmunoprecipitation. Chromatin immunoprecipitation (ChIP) and sequential ChIP analyses demonstrated Sp1-dependent binding of HDAC4 to the proximal p21 promoter, likely directed through the HDAC4 -HDAC3-N-CoR/SMRT corepressor complex. Consistent with increased transcription, HDAC4 or SMRT down-regulation resulted in increased histone H3 acetylation at the proximal p21 promoter locus. These studies identify HDAC4 as a novel regulator of colon cell proliferation through repression of p21. INTRODUCTIONThe acetylation of lysine residues in histones, and/or of transcription factors, is an important posttranslational mechanism of transcriptional regulation (Peterson and Laniel, 2004). Histone deacetylases (HDACs) catalyze the deacetylation of histone and nonhistone substrates, and in general act to repress transcription as part of larger corepressor complexes (Glozak et al., 2005;Yang and Gregoire, 2005). Eighteen mammalian HDACs have been identified to date, and they are grouped into four classes based on their respective homology to yeast deacetylases (Bolden et al., 2006). The class II HDACs can be further subdivided into class IIa (HDAC4, and class , based on the presence in class IIa members of conserved motifs in the N-terminal domain, and extended C terminal tails, that are essential in regulating their function (Yang and Gregoire, 2005).HDACs have emerged as critical regulators of cell growth, differentiation, and apoptotic programs (Bolden et al., 2006). A large body of literature indicates that HDAC inhibitors induce cell cycle arrest, differentiation, and apoptosis in colon cancer cell lines in vitro (Heerdt et al., 1994;Mariadason et al., 1997;Archer et al., 1998;Litvak et al., 1998;Mariadason et al.,...

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confidence: 75%

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confidence: 90%

Section: Introductionmentioning

confidence: 99%

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HDAC4 Promotes Growth of Colon Cancer Cells via Repression of p21

Wilson

Byun

Nasser

et al. 2008

MBoC

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189

172

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“…Multiple HDAC enzymes have been identified, of which HDAC1 to HDAC10 are expressed in malignant cells (16)(17)(18)(19)(20)(21)(22)(23)(24)(25)(26)(27). To understand the spectrum of HDACs inhibited by droxinostat and determine whether selective HDAC inhibition is sufficient to sensitize cells to FAS and TRAIL, we examined the spectrum of HDAC enzymes inhibited by droxinostat.…”

Section: Droxinostat Selectively Inhibits Hdac3 Hdac6 and Hdac8mentioning

confidence: 99%

Selective Inhibition of Histone Deacetylases Sensitizes Malignant Cells to Death Receptor Ligands

Wood

Dalili

Simpson

et al. 2010

Molecular Cancer Therapeutics

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Evasion of death receptor ligand-induced apoptosis represents an important contributor to cancer development and progression. Therefore, molecules that restore sensitivity to death receptor stimuli would be important tools to better understand this biological pathway and potential leads for therapeutic adjuncts. Previously, the small-molecule 4-(4-chloro-2-methylphenoxy)-N-hydroxybutanamide (that we propose be named droxinostat) was identified as a chemical sensitizer to death receptor stimuli, decreasing the expression of the caspase-8 inhibitor FLIP. However, the direct targets of droxinostat were unknown. To better understand the mechanism of action of droxinostat and highlight new strategies to restore sensitivity to death receptor ligands, we analyzed changes in gene expression using the Connectivity Map after treating cells with droxinostat. Changes in gene expression after droxinostat treatment resembled changes observed after treatment with histone deacetylase (HDAC) inhibitors. Therefore, we examined the effects of droxinostat on HDAC activity and showed that it selectively inhibited HDAC3, HDAC6, and HDAC8 and that inhibition of these HDACs was functionally important for its ability to sensitize cells to death ligands. Thus, we have identified a selective HDAC inhibitor and showed that selective HDAC inhibition sensitizes cells to death ligands, thereby highlighting a new mechanism to overcome resistance to death receptor ligands. Mol Cancer Ther; 9(1); 246-56. ©2010 AACR.

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“…Disease Specific patient Survival (DSS) in serous, mucinous, and clear cell carcinomas had no statistical significant but in endometrioid ovarian cancer had negative impact on patient survival [46,47]. The use of the biomarker for hyperacetylation of histones [both in blood lymphocytes and tumor cells] has been useful as a guide to target specificity in early studies of HDAC inhibitors, and this biomarker has been the most extensively developed so far.…”

Section: Brain Tumors Hdac9 Hdac11mentioning

confidence: 99%

The Role of Histone Deacetylase (HDAC) as a Biomarker in Cancer

Moradzadeh¹,

Tabarraei²,

Sadeghnia³

2015

J Mol Biomark Diagn

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Histone acetylases [HAT] and histone deacetylases [HDACs] are responsible for the addition and removal of acetyl-groups to or from specific lysine residues located within histone tails and a number of non-histone proteins. HDACs, as one of the epigenetic mechanisms, play a central role in the regulation of cellular properties that related to development and progression of cancer. Recently, researches began to focus on the expression patterns of HDAC isoforms as a biomarker in cancer. It could be used to find new agents that are very effective in inducing apoptosis, differentiation, and/or cell growth arrest in neoplasia. Approximately, all of studies showed HDAC expression level differ in human tumors. For example, in most tumor entities class I HDAC expression was higher in late stage, high-grade tumors with strong proliferative activity and Class II HDACs down regulated in human tumors and high expression in some tumors was linked to a better prognosis. Thus, this factor allowed to opens new possibilities for a molecularly targeted approach to treatment.

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Drug-induced inactivation or gene silencing of class I histone deacetylases suppresses ovarian cancer cell growth: Implications for therapy

Cited by 97 publications

References 29 publications

HDAC4 Promotes Growth of Colon Cancer Cells via Repression of p21

HDAC4 Promotes Growth of Colon Cancer Cells via Repression of p21

Selective Inhibition of Histone Deacetylases Sensitizes Malignant Cells to Death Receptor Ligands

The Role of Histone Deacetylase (HDAC) as a Biomarker in Cancer

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