<i>In vivo</i> anti‐myeloma activity and modulation of gene expression profile induced by valproic acid, a histone deacetylase inhibitor

Neri, Paola; Tagliaferri, Pierosandro; Martino, Maria Teresa Di; Calimeri, Teresa; Amodio, Nicola; Bulotta, Alessandra; Ventura, Monica; Eramo, Pasqua Orietta; Viscomi, Caterina; Arbitrio, Mariamena; Rossi, Marco; Caraglia, Michele; Munshi, Nikhil C.; Anderson, Kenneth C.; Tassone, Pierfrancesco

doi:10.1111/j.1365-2141.2008.07387.x

Cited by 61 publications

(58 citation statements)

References 63 publications

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“…In vitro exposure of interleukin-6-dependent or -independent MM cells to VPA inhibits cell proliferation in a time-and dose-dependent manner and induces apoptosis (20). In a cohort of severe combined immunodeficienct mice bearing human MM xenografts, VPA was observed to induce tumor growth inhibition and improve survival rates in treated animals compared with controls (20). ATO has long been used as a therapeutic agent.…”

Section: Discussionmentioning

confidence: 99%

Synergistic effects of valproic acid and arsenic trioxide on RPMI8226 cells in vitro and the possible underlying mechanisms

Wang

Zhang

2012

Molecular Medicine Reports

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Abstract. The aim of the present study was to investigate the synergistic effects of valproic acid (VPA) and arsenic trioxide (ATO) on the proliferation of RPMI8226 cells and the possible underlying mechanisms. Cell apoptosis was assessed by flow cytometry. The mRNA expression levels were analyzed by semi-quantitative polymerase chain reaction, and the protein expression levels were analyzed by western blotting. The histone acetylation and methylation states of the gene promoters were detected using a chromatin immunoprecipitation technique. The apoptotic rates of the RPMI8226 cells in the combined drug groups were significantly increased compared with those of the single drug groups (P<0.05). The mRNA and protein expression levels of Bcl-2 and the expression levels of HDAC1 mRNA and H3K9me2 protein decreased significantly in the combined groups compared with the single drug groups. The mRNA and protein expression levels of Bax, Caspase 8, Caspase 9 and LSD1, and the protein expression of acetylated H3 increased significantly in the combination groups compared with the single drug groups. Histone methylation and acetylation of the Bcl-2 and bax gene promoters were increased in the combination groups compared with the single drug groups. VPA and ATO had synergistic effects on the proliferation of RPMI8226 cells, which may have been associated with the decreased expression of Bcl-2 and the increased expression levels of Bcl-2-associated X protein, Caspase 8 and Caspase 9. Therefore, the expression levels of the Bcl-2 gene family may have been regulated by the levels of gene promoter methylation and acetylation. IntroductionMultiple myeloma (MM) is a plasma cell disorder, characterized by anemia, renal disease, lytic bone disease, and immune dysfunction. MM is one of the most common types of hematological malignancy in China (1). Although currently approved treatments for newly diagnosed MM, including high-dose chemotherapy followed by autologous transplantation, and novel drugs, including proteasome inhibitors and immunomodulatory agents (IMiDs), have led to increased survival rates, the majority of patients will eventually relapse and become refractory to treatment (2). Therefore, patients with relapsed or refractory MM have an unmet requirement for safe and efficacious novel therapies.Arsenic trioxide (ATO) has been suggested as an option for the treatment of relapsing or refractory MM. In vitro, ATO has been found to induced myeloma cell apoptosis, and monotherapy with ATO results in partial response rates between 0 and 17%, and minimal responses between 7 and 33%, resulting in mean overall response rates of 30% for treatment of myeloma (3-5).In order to improve the treatment response rates in patients with MM, ATO has been combined with other novel drugs, including proteasome inhibitors, IMiDs and dexamethsone, for the treatment of MM. The overall response rates in these combined regimens vary widely between 12 and 100% (6-8). It is necessary to identify novel combinations of ATO with other drugs, to offer nov...

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Section: Discussionmentioning

confidence: 99%

Synergistic effects of valproic acid and arsenic trioxide on RPMI8226 cells in vitro and the possible underlying mechanisms

Wang

Zhang

2012

Molecular Medicine Reports

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“…12 Although a genome-wide comparison is not possible, the gene pattern modulated by ITF2357 is in line with that previously observed in MM1 cells treated with other HDAC K. Todoerti et al 266 haematologica | 2010; 95(2) inhibitors. 29,30 Indeed several genes shown here, such as CD138, CD126, IGF1, TNFRSF1, MYB, CDK3, CDK1B, CDK1A (p21), CDKN1C (p57), CDKN2D (p19) and APAF1, have been previously identified to be modulated in MM cells by the pan-HDAC inhibitor SAHA. 29 Interestingly, CDK1A, CDKN1C, CDKN1B (p27), MYC, BID and CD138 have also been described to be modulated in MM cells by the class I specific HDAC inhibitor valproic acid.…”

Section: Discussionmentioning

confidence: 99%

“…29 Interestingly, CDK1A, CDKN1C, CDKN1B (p27), MYC, BID and CD138 have also been described to be modulated in MM cells by the class I specific HDAC inhibitor valproic acid. 30 A full understanding of the role of the various HDAC isoforms in regulating specific sets of genes does, however, await further analyses with isoform-specific inhibitors using identical cellular targets and time points.…”

Section: Discussionmentioning

confidence: 99%

Pleiotropic anti-myeloma activity of ITF2357: inhibition of interleukin-6 receptor signaling and repression of miR-19a and miR-19b

et al. 2009

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The online version of this article has a supplementary appendix. BackgroundThe histone deacetylase inhibitor ITF2357 has potent cytotoxic activity in multiple myeloma in vitro and has entered clinical trials for this disease. Design and MethodsIn order to gain an overall view of the activity of ITF2357 and identify specific pathways that may be modulated by the drug, we performed gene expression profiling of the KMS18 multiple myeloma cell line treated with the drug. The modulation of several genes and their biological consequence were verified in a panel of multiple myeloma cell lines and cells freshly isolated from patients by using polymerase chain reaction analysis and western blotting. ResultsOut of 38,500 human genes, we identified 140 and 574 up-regulated genes and 102 and 556 down-modulated genes at 2 and 6 h, respectively, with a significant presence of genes related to transcription regulation at 2 h and to cell cycling and apoptosis at 6 h. Several of the identified genes are particularly relevant to the biology of multiple myeloma and it was confirmed that ITF2357 also modulated their encoded proteins in different multiple myeloma cell lines. In particular, ITF2357 down-modulated the interleukin-6 receptor α (CD126) transcript and protein in both cell lines and freshly isolated patients' cells, whereas it did not significantly modify interleukin-6 receptor β (CD130) expression. The decrease in CD126 expression was accompanied by decreased signaling by interleukin-6 receptor, as measured by STAT3 phosphorylation in the presence and absence of interleukin-6. Finally, the drug significantly down-modulated the MIRHG1 transcript and its associated microRNA, miR-19a and miR-19b, known to have oncogenic activity in multiple myeloma. ConclusionsITF2357 inhibits several signaling pathways involved in myeloma cell growth and survival.Key words: pleiotropic anti-myeloma, ITF2357, interleukin-6 receptor, miR-19a, miR-19b. -19a and miR-19b. Haematologica. 2010; 95:260-269. doi:10.3324/haematol.2009 This is an open-access paper.Pleiotropic anti-myeloma activity of ITF2357: inhibition of interleukin-6 receptor signaling and repression of miR-19a and miR-19b

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“…This is in line with other studies, demonstrating that upregulation of p21 Waf1 is a hallmark for the HDACi-induced cell cycle arrest. 25,26,28,[43][44][45] This corresponds with the anti-proliferative activity of JNJ-26481585. However at 72 h incubation, cell cycle arrest is lost, most likely because of the large increase of apoptotic cells.…”

Section: Discussionmentioning

confidence: 99%

The effects of JNJ-26481585, a novel hydroxamate-based histone deacetylase inhibitor, on the development of multiple myeloma in the 5T2MM and 5T33MM murine models

et al. 2009

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Multiple myeloma (MM) is a B-cell malignancy, which often remains incurable because of the development of drug resistance governed by the bone marrow (BM) microenvironment. Novel treatment strategies are therefore urgently needed. In this study, we evaluated the anti-MM activity of JNJ-26481585, a novel 'second-generation' pyrimidyl-hydroxamic acid-based histone deacetylase inhibitor, using the syngeneic murine 5TMM model of MM. In vitro, JNJ-26481585 induced caspase cascade activation and upregulation of p21, resulting in apoptosis and cell cycle arrest in the myeloma cells at low nanomolar concentrations. Similar results could be observed in BM endothelial cells using higher concentrations, indicating the selectivity of JNJ-26481585 toward cancer cells. In a prophylactic and therapeutic setting, treatment with JNJ-26481585 resulted in an almost complete reduction of the tumor load and a significant decrease in angiogenesis. 5T2MM-bearing mice also developed a MM-related bone disease, characterized by increased osteoclast number, development of osteolytic lesions and a reduction in cancellous bone. Treatment of these mice with JNJ-264815 significantly reduced the development of bone disease. These data suggest that JNJ-26481585 has a potent anti-MM activity that can overcome the stimulatory effect of the BM microenvironment in vivo making this drug a promising new anti-MM agent.

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In vivo anti‐myeloma activity and modulation of gene expression profile induced by valproic acid, a histone deacetylase inhibitor

Cited by 61 publications

References 63 publications

Synergistic effects of valproic acid and arsenic trioxide on RPMI8226 cells in vitro and the possible underlying mechanisms

Synergistic effects of valproic acid and arsenic trioxide on RPMI8226 cells in vitro and the possible underlying mechanisms

Pleiotropic anti-myeloma activity of ITF2357: inhibition of interleukin-6 receptor signaling and repression of miR-19a and miR-19b

The effects of JNJ-26481585, a novel hydroxamate-based histone deacetylase inhibitor, on the development of multiple myeloma in the 5T2MM and 5T33MM murine models

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