Comparative effects of lovastatin on mammary and prostate oncogenesis in transgenic mouse models

Shibata, Masa‐Aki; Kavanaugh, Claudine; Shibata, Eiko; Abe, Hideaki; Nguyên, Philippe; Otsuki, Yoshinori; Trepel, Jane B.; Green, Jeffrey E.

doi:10.1093/carcin/24.3.453

Cited by 87 publications

(72 citation statements)

References 27 publications

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“…In general, various cancers are sensitive to statin treatment (33)(34)(35). Similarly, ovarian cancer cells may be sensitive to simvastatin treatment (12).…”

Section: Discussionmentioning

confidence: 99%

“…In addition, statins induce apoptosis through both the extrinsic and intrinsic pathways. Shibata et al (34) reported that lovastatin induced p53-independent mitochondrial-mediated apoptosis in a mouse mammary carcinoma. The sensitivity of different cell types to statin-induced apoptosis varies; acute myeloid leukemic and neuroblastoma cells are more sensitive than acute lymphoblastic leukemic cells (40).…”

Section: Discussionmentioning

confidence: 99%

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Statin-mediated reduction of osteopontin expression induces apoptosis and cell growth arrest in ovarian clear cell carcinoma

Matsuura

Suzuki²,

Suzuki³

et al. 2010

Oncol Rep

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Abstract. Poor prognosis in ovarian clear cell carcinoma is associated with the expression of a defined set of proteins including osteopontin (OPN) and integrin. Statins, a family of 3-hydroxy-3-methylglutaryl CoA reductase inhibitors, are currently being investigated for the treatment and prevention of cancer. In this study, we investigated the effects of simvastatin on ovarian clear cell carcinoma (OCCC) cells in vitro and in vivo and elucidated the mechanism of drug action. Changes in OPN gene expression were determined by real-time RT-PCR, and an MTT assay was performed to determine effects on cell proliferation. Finally, a xenograft tumor model was constructed to evaluate the effects of simvastatin on cell proliferation and apoptosis in vivo. According to our experimental results, OPN is an important protein in OCCC. Simvastatin inhibited OCCC cell proliferation, and the inhibition rate was approximately 40% to 50% after treatment with 10 μM simvastatin for 48 h. In the xenograft studies, simvastatin treatment resulted in a significant growth inhibition. Furthermore, the mice treated with simvastatin survived significantly longer compared to the control groups. In conclusion, simvastatin has anticancer effects in vitro and in vivo. Further confirmation of the anticancer effects of statins in future studies will increase the scope for OCCC treatment.

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“…In general, various cancers are sensitive to statin treatment (33)(34)(35). Similarly, ovarian cancer cells may be sensitive to simvastatin treatment (12).…”

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Statin-mediated reduction of osteopontin expression induces apoptosis and cell growth arrest in ovarian clear cell carcinoma

Matsuura

Suzuki²,

Suzuki³

et al. 2010

Oncol Rep

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“…The indirect approach can be through the agents capable of inducing the expression of cyclin inhibitors or via peptides mimicking the effects of these inhibitors. In a number of studies, the indirect effect of cyclin inhibitor p21 has been demonstrated, either overexpression via viral and nonviral vectors (1)(2)(3)(4)(5)(6) or through the induction of p21 by different therapeutic agents (7)(8)(9)(10). We have demonstrated previously that anti-inflammatory/immunosuppressive drugs, e.g., cyclosporine (CsA) 2 , tacrolimus (TAC), and sirolimus (SRL) (11)(12)(13), induce the expression of cyclin inhibitor p21.…”

mentioning

confidence: 99%

Recombinant p21 Protein Inhibits Lymphocyte Proliferation and Transcription Factors

Khanna

Plummer

Nilakantan

et al. 2005

The Journal of Immunology

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Cellular proliferation determines the events leading to the initiation and development of inflammation, immune activation, cancer, atherogenesis, and other disorders associated with aberrant cell proliferation. Cyclin inhibitor p21 plays a unique role in limiting cell cycle progression. However, its effectiveness can only be demonstrated with direct in vitro and in vivo delivery to control aberrant proliferation. We demonstrate that using a protein-transducing domain p21 protein a) localizes within the nuclear compartments of cells, b) interacts with transcription factors, NF-κB, and NFATs (NFATc and NFATp), and c) inhibits lymphocyte proliferation and expression of proinflammatory cytokines. This study using lymphocyte proliferation as a model suggests that the recombinant p21 protein can directly be delivered as a therapeutic protein to provide a novel, viable, and powerful strategy to limit proliferation, inflammation, alloimmune activation, cancer, and vascular proliferative disorders such as atherosclerosis.

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“…Wu et al applied 5 μmol/L lovastatin to treat CHO cells for 32 hours and the proportion of cells in G1 phase was 90% (Wu and Gilbert, 2000). In addition, lovastatin at 10 and 20 μmol/L was applied to treat M6 cells and MCF-1 cells for 24 and 33 hours, respectively, and 78% and 77~96% of cells were identified to be in the G1 phase (Gupta et al, 2003;Shibata et al, 2003). Treatment of Pr14 cells and Pc-3M cells with 10 μmol/L lovastatin for 24 hours and 24~48 hours can achieve 82% and 68~90% of cells in G1 phase, respectively (Park et al, 2001;Shibata et al, 2003).…”

Section: Discussionmentioning

confidence: 99%

“…In addition, lovastatin at 10 and 20 μmol/L was applied to treat M6 cells and MCF-1 cells for 24 and 33 hours, respectively, and 78% and 77~96% of cells were identified to be in the G1 phase (Gupta et al, 2003;Shibata et al, 2003). Treatment of Pr14 cells and Pc-3M cells with 10 μmol/L lovastatin for 24 hours and 24~48 hours can achieve 82% and 68~90% of cells in G1 phase, respectively (Park et al, 2001;Shibata et al, 2003). Treatment of T-24 cells with 30 μmol/L lovastatin may achieve 80% of cells in G1 phase and about 70~90% of Calu-1 cells were identified to be in the G1 phase following treatment with 30 μmol/L lovastatin (Jakobisiak et al, 1991;Vogt et al, 1997).…”

Section: Discussionmentioning

confidence: 99%

Lovastatin induces G1-phase synchronization of HEC-1-A cells and JEC cells

Shen

Yang

et al. 2013

Bangladesh J Pharmacol

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MaterialsHuman endometrial cancer cell lines (HEC-1-A cells and JEC cells) were preserved in our lab. DMEM low glucose, fetal bovine serum (FBS) (GIBCO), trypsinThis work is licensed under a Creative Commons Attribution 3.0 License. You are free to copy, distribute and perform the work. You must attribute the work in the manner specified by the author or licensor. AbstractOur study investigated lovastatin-induced G1 phase synchronization of HEC-1-A cells and JEC cells and the cell cycle progression after desynchronization of these cells. HEC-1-A cells and JEC cells were treated with by lovastatin and the proportion of cells in G1 phase was detected. Both cell types were incubated with lovastatin and the synchronization was determined. The cell cycle progression of both cell types was investigated. The proportion of Both cell types in G1 phase was 87.9 ± 0.7% and 85.0 ± 0.8%, respectively. At 20 and 16 hours after G1-phase desynchronization, the proportion of cells in S phase reached a maximal level and that in G1 phase was at the minimal level for HEC-1-A cells and JEC cells, respectively. Thus, at 20 and 16 hours after desynchronization, the proportion of cells in S phase was the highest and that in G1 phase the lowest for HEC-1-A cells and JEC cells, respectively. Article Info

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Comparative effects of lovastatin on mammary and prostate oncogenesis in transgenic mouse models

Cited by 87 publications

References 27 publications

Statin-mediated reduction of osteopontin expression induces apoptosis and cell growth arrest in ovarian clear cell carcinoma

Statin-mediated reduction of osteopontin expression induces apoptosis and cell growth arrest in ovarian clear cell carcinoma

Recombinant p21 Protein Inhibits Lymphocyte Proliferation and Transcription Factors

Lovastatin induces G1-phase synchronization of HEC-1-A cells and JEC cells

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