YM155 Reverses Statin Resistance in Renal Cancer by Reducing Expression of Survivin

Nitta, Takashi; Koike, Hidekazu; Miyao, Takeshi; Miyazawa, Yoshiyuki; Kato, Haruo; Furuya, Yasubumi; Sekine, Yoshitaka; Suzuki, Kazuhiro

doi:10.21873/anticanres.11291

Cited by 7 publications

(4 citation statements)

References 29 publications

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“…Furthermore, YM155 significantly enhanced the antitumor effects of rapamycin in these cells. Additionally, we found that, in the statin-resistant renal cell clear cell carcinoma cell line, Caki-1-StaR, survivin knockdown by siRNA or YM155 significantly reversed simvastatin resistance in vitro (17). These findings prompted us to confirm the effects of survivin inhibition in a CRPC model.…”

Section: Discussionmentioning

confidence: 79%

YM155 Reverses Cabazitaxel Resistance in Castration-resistant Prostate Cancer by Reducing Survivin Expression

et al. 2020

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Background/Aim: The purpose of the present study was to clarify whether treatment with YM155, a novel small-molecule inhibitor of survivin, reversed cabazitaxel resistance in castration-resistant prostate cancer (CRPC). Materials and Methods: Cabazitaxel resistance was induced in the castration-resistant prostate cancer cell line, 22Rv1-CR. In vitro and in vivo models were used to test the efficacy of YM155 and cabazitaxel. Results: Survivin gene expression was significantly higher in 22Rv1-CR than its parent cells (22Rv1). In 22Rv1-CR cells, YM155 significantly reduced expression of the survivin gene in a concentration-dependent manner. YM155 alone was poorly effective; however, it significantly enhanced the anticancer effects of cabazitaxel on 22Rv1-CR in vitro and in vivo. Conclusion: Inhibition of survivin by YM155 overcomes cabazitaxel resistance in CRPC cells.Cabazitaxel was more efficacious in terms of producing a significant difference in patients with castration-resistant prostate cancer (CRPC) compared with the control group in the TROPIC trial (1). Hence, cabazitaxel is now employed as the standard treatment for most patients with CRPC. However, treatment outcomes are not always completely successful. Thus, the development of a new therapeutic regimen is required.Survivin is a member of a family of eight different proteins that function as inhibitors of apoptosis (2). In 1997, Altieri et al. reported, for the first time, that survivin controlled apoptosis in cancer cells (3). It was also reported that survivin is overexpressed in several kinds of cancer and is involved in the survival of cancer cells and cell division.Conversely, cancer cell apoptosis is induced when the function of survivin is restrained. Additionally, because survivin expression level correlates with malignant disease prognosis and drug resistance, it is considered a potential target of future cancer therapeutics.A novel small-molecule inhibitor of survivin, YM155, was identified by cell-based high-throughput screening (4). YM155 suppresses the transactivation of survivin by directly binding to its promoter (5). Subsequently, Cheng et al. reported that YM155-mediated inhibition of survivin expression occurs, at least in part, through inhibition of survivin transcription by disrupting Sp1 interaction with the -149 to -71 region in the survivin core promoter (6).YM155 exhibits potent antitumor activity in vitro, and induces tumor regression in established non-small cell lung cancer, non-Hodgkin lymphoma, melanoma, and hormonerefractory prostate cancer xenografts (4, 7-9). The anticancer efficacy of YM155 as monotherapy or in combination with docetaxel (10) or platinum compounds, such as cisplatin and carboplatin (11) has been shown in Xenograft models (4,12).The purpose of this study was to determine the efficacy of YM155 and whether YM155 treatment could reverse acquired cabazitaxel resistance in the prostate cancer cell line 22Rv1-CR both in vitro and in vivo. Materials and MethodsCells and chemicals. The human prostate cancer cell l...

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Section: Discussionmentioning

confidence: 79%

YM155 Reverses Cabazitaxel Resistance in Castration-resistant Prostate Cancer by Reducing Survivin Expression

et al. 2020

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“…Several approaches, including the use of the transcriptional inhibitor sepantronium bromide (YM155), have been designed to target survivin (15)(16)(17). However, recent studies have revealed that an improvement in the response rate was not observed when YM155 was added to the combination therapy of carboplatin and paclitaxel for progressive nonsmall cell lung cancer in Phase I/II trials (18).…”

Section: Discussionmentioning

confidence: 99%

Inhibition of Survivin by Adenovirus Vector Enhanced Paclitaxel-induced Apoptosis in Breast Cancer Cells

Tanaka

Uchida

2018

Anticancer Res

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“…(22-24) YM-155 has been reported to overcome drug resistance (e.g. statins (16,(25)(26)(27) docetaxel (28)), improve efficacy of diverse therapies including hypericin-mediated photodynamic therapies (29) and on its own merit, induces apoptosis, reduces colony formation, attenuates invasion and growth of xenograft tumors in nude mice (30)(31)(32)(33). While reduction of survivin by YM-155 is believed to be a foremost mechanism of action, other biochemical targets for this drug are continually being reported in the literature.…”

Section: Discussionmentioning

confidence: 99%

Effects of Sepantronium Bromide (YM-155) on the Whole Transcriptome of MDA-MB-231 Cells: Highlight on Impaired ATR/ATM Fanconi Anemia DNA Damage Response

Mazzio

Lewis

Elhag

et al. 2018

Cancer Genomics Proteomics

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Sepantronium bromide (YM-155) is believed to elicit apoptosis and mitotic arrest in tumor cells by reducing (BIRC5, survivin) mRNA. In this study, we monitored changes in survivin mRNA and protein after treating MDA-MB-231 cells with YM-155 concurrent with evaluation of whole transcriptomic (WT) mRNA and long intergenic non-coding RNA at 2 time points: 8 h sub-lethal (83 ng/mL) and 20 h at the LC (14.6 ng/mL). The data show a tight association between cell death and the precipitating loss of survivin protein and mRNA (-2.67 fold-change (FC), p<0.001) at 20 h, questioning if the decline in survivin is attributed to cell death or drug impact. The meager loss of survivin mRNA was overshadowed by enormous differential change to the WT in both magnitude and significance for over 2000 differentially up/down-regulated transcripts: (+22 FC to -12 FC, p<0.001). The data show YM-155 to up-regulate transcripts in control of circadian rhythm (NOCT, PER, BHLHe40, NFIL3), tumor suppression (SIK1, FOSB), histone methylation (KDM6B) and negative feedback of NF-kappa B signaling (TNFAIP3). Down-regulated transcripts by YM-155 include glucuronidase (GUSBP3), numerous micro-RNAs, DNA damage repair elements (CENPI, POLQ, RAD54B) and the most affected system was the ataxia-telangiectasia mutated (ATM)/Fanconi anemia E3 monoubiquitin ligase core complexes (FANC transcripts - A/B/E/F/G/M), FANC2, FANCI, BRCA1, BRCA2, RAD51, PALB2 gene and ATR (ATM- and Rad3-Related) pathway. In conclusion, these findings suggest that a primary target of YM-155 is the loss of replicative DNA repair systems.

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YM155 Reverses Statin Resistance in Renal Cancer by Reducing Expression of Survivin

Cited by 7 publications

References 29 publications

YM155 Reverses Cabazitaxel Resistance in Castration-resistant Prostate Cancer by Reducing Survivin Expression

YM155 Reverses Cabazitaxel Resistance in Castration-resistant Prostate Cancer by Reducing Survivin Expression

Inhibition of Survivin by Adenovirus Vector Enhanced Paclitaxel-induced Apoptosis in Breast Cancer Cells

Effects of Sepantronium Bromide (YM-155) on the Whole Transcriptome of MDA-MB-231 Cells: Highlight on Impaired ATR/ATM Fanconi Anemia DNA Damage Response

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