Mithramycin A sensitizes cancer cells to TRAIL-mediated apoptosis by down-regulation of <i>XIAP</i> gene promoter through Sp1 sites

Lee, Tae Jin; Jung, Eun Mi; Lee, Jung Tae; Kim, Shin; Park, Jong Wook; Choi, Kyeong Sook; Kwon, Taeg Kyu

doi:10.1158/1535-7163.mct-06-0426

Cited by 66 publications

(51 citation statements)

References 27 publications

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“…Our results are con- sistent with a previous report showing that two putative SP1 binding sites (Ϫ144 and Ϫ25 bp) with the 5Ј-untranslated region were involved in the SP1-mediated regulation of XIAP expression (11). Based on our results from the ChIP assay, SP1 appears to be a major participant in transcription factor binding to the GC-box site of the XIAP promoter and is critically involved in down-regulating XIAP transcription upon ISO treatment.…”

Section: Discussionsupporting

confidence: 89%

“…5F). Considering that there are two SP1 binding sites between Ϫ214 and ϩ60 (Ϫ144 and Ϫ25) and that the previous report (11) showed that XIAP promoter activity is significantly decreased by double mutation of two SP1 sites at Ϫ144 and Ϫ25, we suggest that ISO down-regulation of XIAP transcription is mediated by its targeting and inhibiting of SP1 expression, transactivation, and specific binding to SP1 binding sites, particularly the two SP1 binding sites at Ϫ144 and Ϫ25 in the XIAP promoter region as shown in Fig. 5G.…”

Section: Iso Treatment Suppresses Transcription Factor Sp1 Expressionmentioning

confidence: 70%

See 1 more Smart Citation

The Chinese Herb Isolate Isorhapontigenin Induces Apoptosis in Human Cancer Cells by Down-regulating Overexpression of Antiapoptotic Protein XIAP

Fang

Hou

et al. 2012

Journal of Biological Chemistry

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Background:The anti-cancer activity and mechanisms of isorhapontigenin (ISO) have never been explored. Results: ISO exhibited an anti-cancer activity accompanied by apoptotic induction and XIAP down-regulation through attenuation of SP1 expression. Conclusion: ISO is an active anti-cancer compound by inducing apoptosis via down-regulation of SP1/XIAP pathway. Significance: Current studies identify a new promising active compound for therapy of human cancers with XIAP overexpression.

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Section: Discussionsupporting

confidence: 89%

Section: Iso Treatment Suppresses Transcription Factor Sp1 Expressionmentioning

confidence: 70%

The Chinese Herb Isolate Isorhapontigenin Induces Apoptosis in Human Cancer Cells by Down-regulating Overexpression of Antiapoptotic Protein XIAP

Fang

Hou

et al. 2012

Journal of Biological Chemistry

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“…RT-PCR analysis was done as previously described [13]. The cDNAs for DR5 and actin were amplified by PCR with specific primers.…”

Section: Rna Isolation and Reverse Transcriptase-polymerase Chain Reamentioning

confidence: 99%

“…Chromatin immunoprecipitation assays were done as previously described [13]. Purified DNA was subjected to PCR with primers specific for a region (+1 to +196) relative to the proposed transcriptional start site in the c-FLIP promoter spanning a putative NF-κB binding site.…”

Section: Chromatin Immunoprecipitation (Chip) Assaymentioning

confidence: 99%

Withaferin A sensitizes TRAIL-induced apoptosis through reactive oxygen species-mediated up-regulation of death receptor 5 and down-regulation of c-FLIP

Lee

Min

et al. 2009

Free Radical Biology and Medicine

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“…Mithramycin A was previously used to demonstrate the specificity of Sp1 binding to target promoters (22,23). To further confirm the dependence of RON gene expression on Sp1, additional experiments were performed by treating MDA MB 231 cells with mithramycin A, an inhibitor of Sp1 binding.…”

Section: Mithramycin a Or Sirna Sp1 Knock-down Blocks Ron Gene Expresmentioning

confidence: 99%

Regulation of RON Tyrosine Kinase-mediated Invasion of Breast Cancer Cells

Thangasamy

Rogge

Ammanamanchi

2008

Journal of Biological Chemistry

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Macrophage-stimulating protein (MSP)2 is the only known ligand for RON (recepteur d'origine nantais). MSP is an 80 kDa heterodimer consisting of a 53 kDa ␣ chain and a 30-kDa ␤ chain linked by a disulfide bond. The ␤ chain of MSP binds to RON. MSP belongs to the plasminogen-prothrombin gene family (1, 2). MSP gene knock-out in mice is not lethal, indicating that MSP is not required for embryonic development and growth (3). Besides macrophages, MSP is expressed in a variety of epithelial cells. RON is initially synthesized as a single chain precursor, 170-kDa pro-RON, which is subsequently cleaved into 40-kDa ␣ chain and 150-kDa ␤ chain. The ␣ chain is completely extracellular, whereas the ␤ chain traverses the cell membrane and contains the intracellular tyrosine kinase (1). The C-terminal of RON regulates its kinase activity (4). RON forms either homodimers or heterodimers with other receptors such as c-Met and epidermal growth factor receptor (5-7). In addition to macrophages, RON is also expressed in multiple epithelial cells both malignant and nonmalignant. Homozygous deletion of RON was embryonically lethal. However, RON heterozygous mice mature normally except for an inappropriate inflammatory response (8, 9). The RON protein is regulated through c-Cbl ubiquitin ligase binding to phosphorylated RON leading to endocytosis and the subsequent degradation of RON (10).Abnormal expression of RON was reported in various cancers of epithelial origin. However, fibroblasts do not express RON. RON is moderately expressed in normal colorectal mucosa but significantly elevated in a majority of primary human colorectal adenocarcinoma samples (11). RON protein accumulation was reported to induce autophosphorylation of RON tyrosine kinase receptor and transduces signals that regulate tumorigenic activities of colon cancer cells (12). In nonsmall cell lung cancer cell lines, RON overexpression was reported in a majority of the cell lines examined. In addition, these cell lines expressed high levels of MSP ligand (13). The combination of RON overexpression and activation by MSP leads to increased invasion and resistance to apoptosis. These tumors supported by either autocrine or paracrine effects may acquire a survival advantage because of increased activation of the RON receptor by the local secretion of MSP.Altered RON expression was noticed in bladder and ovarian cancers. RON expression was positively associated with tumor size, stage, and grade in bladder carcinomas (14). The majority of ovarian carcinoma samples showed up-regulation in RON expression with a mix of cytoplasmic and membrane staining (5). Co-expression of MSP with RON was observed in ovarian carcinomas, providing a selective growth advantage and subsequent tumor progression. RON overexpression and not mutations is associated with head and neck squamous cell carcinomas (15). Normal breast cells and benign lesions (adenomas and papillomas) express relatively low levels of RON. However, RON is highly expressed in tumor specimens (1). Further, increased RON e...

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Mithramycin A sensitizes cancer cells to TRAIL-mediated apoptosis by down-regulation of XIAP gene promoter through Sp1 sites

Cited by 66 publications

References 27 publications

The Chinese Herb Isolate Isorhapontigenin Induces Apoptosis in Human Cancer Cells by Down-regulating Overexpression of Antiapoptotic Protein XIAP

The Chinese Herb Isolate Isorhapontigenin Induces Apoptosis in Human Cancer Cells by Down-regulating Overexpression of Antiapoptotic Protein XIAP

Withaferin A sensitizes TRAIL-induced apoptosis through reactive oxygen species-mediated up-regulation of death receptor 5 and down-regulation of c-FLIP

Regulation of RON Tyrosine Kinase-mediated Invasion of Breast Cancer Cells

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