A novel screen using the Reck tumor suppressor gene promoter detects both conventional and metastasis-suppressing anticancer drugs

Murai, Ryuya; Yoshida, Yoko; Muraguchi, Teruyuki; Nishimoto, Emi; Morioka, Yoshiyuki; Kitayama, Hitoshi; Kondoh, S.; Kawazoe, Yoshinori; Hiraoka, Masahiro; Uesugi, Motonari; Noda, Makoto

doi:10.18632/oncotarget.136

Cited by 28 publications

(14 citation statements)

References 52 publications

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“…In a small number of cell‐based models they were also able to show that DSF suppressed the growth of cells that had metastasized to the lymph nodes and lungs . Consistent with this study, DSF was identified in a large screen for antimetastatic agents using a model of fibrosarcoma . Given that 90% of all cancer deaths are due to metastases it is encouraging that DSF could provide some benefit in cancers that have spread.…”

Section: Repurposing Dsf For Other Cancerssupporting

confidence: 74%

Concise Review: Bullseye: Targeting Cancer Stem Cells to Improve the Treatment of Gliomas by Repurposing Disulfiram

Triscott

Pambid

Dunn³

2015

Stem Cells

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Cancer stem cells (CSCs) are thought to be at the root of cancer recurrence because they resist conventional therapies and subsequently reinitiate tumor cell growth. Thus, targeting CSCs could be the bullseye to successful cancer therapeutics in the future. Brain tumors are some of the most challenging types of cancer to treat and the median survival following the initial diagnosis is 12-18 months. Among the different types of brain tumors, glioblastoma (GBM) is considered the most aggressive and remains extremely difficult to treat. Despite surgery, radiation, and chemotherapy, most patients develop refractory disease. Temozolomide (TMZ) is a chemotherapy used to treat GBM however resistance develops in most patients. The underlying mechanisms for TMZ resistance (TMZ-resistant) involve the expression of DNA repair gene O(6)-methylguanine-DNA methyltransferase. CSC genes such as Sox-2, BMI-1, and more recently Ybox binding protein-1 also play a role in resistance. In order to develop novel therapies for GBM, libraries of small interfering RNAs and off-patent drugs have been screened. Over the past few years, several independent laboratories identified disulfiram (DSF) as an off-patent drug that kills GBM CSCs. Reportedly DSF has several modes of action including its ability to inhibit aldehyde dehydrogenases, E3 ligase, polo-like kinase 1, and NFkB. Due to the fact that GBM is a disease of heterogeneity, chemotherapy with multitargeting properties may be the way of the future. In broader terms, DSF kills CSCs from a range of different cancer types further supporting the idea of repurposing it for "target practice

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Section: Repurposing Dsf For Other Cancerssupporting

confidence: 74%

Concise Review: Bullseye: Targeting Cancer Stem Cells to Improve the Treatment of Gliomas by Repurposing Disulfiram

Triscott

Pambid

Dunn³

2015

Stem Cells

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“…This group developed an original screening method based on the activation of the Reck-promoter fused to the secreted alkaline phosphatase gene [57]. Interestingly, disulfiram, a drug used to cure chronic alcoholism, appeared to be the most potent inducer of RECK, suppressing lung metastasis in a fibrosarcoma mouse model [57]. Interestingly, disulfiram, a drug used to cure chronic alcoholism, appeared to be the most potent inducer of RECK, suppressing lung metastasis in a fibrosarcoma mouse model [57].…”

Section: Additional Pharmacological Targets Derived From Tumor Reversmentioning

confidence: 99%

Lessons from tumor reversion for cancer treatment

Amson¹,

Karp²,

Telerman³

2013

Current Opinion in Oncology

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“…Next, we treated four cell lines that exhibit different RECK methylation patterns [T-47D (RPM+RIM+), MCF7 (RPM-RIM+), BT549 and SKBR3 (RPM-RIM-)] with a RECK-activating anticancer drug, methotrexate (MTX) [35]. T-47D (RPM+) showed lowest sensitivity to this drug (Figure 5C; red line).…”

Section: Resultsmentioning

confidence: 99%

“…A recent study indicate that progesterone inhibits estrogen-induced growth of ER+ breast tumors and that copy number loss of the PR gene is not rare among ER+ breast cancers [37]. The use of DNMT inhibitors in conjunctions with other therapeutic agents, such as anti-estrogens, Cdk inhibitors [38], HDAC inhibitors, or other RECK -activating agents [35], may have potential value in treating such tumors.…”

Section: Discussionmentioning

confidence: 99%

Pattern of RECK CpG methylation as a potential marker for predicting breast cancer prognosis and drug-sensitivity

et al. 2016

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The membrane-anchored glycoprotein RECK negatively regulates multiple metalloproteinases and is frequently downregulated in tumors. Forced RECK expression in cancer cells results in suppression of tumor angiogenesis, invasion, and metastasis in xenograft models. A previous methylome study on breast cancer tissues detected inverse correlation between RECK CpG methylation (in an intron-1 region) and relapse-free survival. In this study, we focused on another region of the RECK CpG island (a promoter/exon-1 region) and found an inverse correlation between its methylation and RECK-inducibility by an HDAC inhibitor, MS275, among a panel of breast cancer cell lines (n=15). In clinical samples (n=62), RECK intron-1 methylation was prevalent among luminal breast cancers as reported previously (26 of 38 cases; 68%) and particularly enriched in tumors of the ER+PR- subclass (10 of 10 cases) and of higher histological grades (Grade 2 and 3; 28 of 43 cases; P=0.006). In about a half of these cases, promoter/exon-1 methylation was absent, and hence, RECK may be inducible by certain drugs such as MS275. Our results indicate the value of combined use of two RECK methylation markers for predicting prognosis and drug-sensitivity of breast cancers.

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A novel screen using the Reck tumor suppressor gene promoter detects both conventional and metastasis-suppressing anticancer drugs

Cited by 28 publications

References 52 publications

Concise Review: Bullseye: Targeting Cancer Stem Cells to Improve the Treatment of Gliomas by Repurposing Disulfiram

Concise Review: Bullseye: Targeting Cancer Stem Cells to Improve the Treatment of Gliomas by Repurposing Disulfiram

Lessons from tumor reversion for cancer treatment

Pattern of RECK CpG methylation as a potential marker for predicting breast cancer prognosis and drug-sensitivity

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