Hyaluronan-CD44 Interaction Activates Stem Cell Marker Nanog, Stat-3-mediated MDR1 Gene Expression, and Ankyrin-regulated Multidrug Efflux in Breast and Ovarian Tumor Cells

Bourguignon, Lilly Y.W.; Peyrollier, Karine; Xia, Weiliang; Gilad, Eli

doi:10.1074/jbc.m800109200

Cited by 398 publications

(403 citation statements)

References 97 publications

Supporting

Mentioning

390

Contrasting

Unclassified

Order By: Relevance

“…We have demonstrated for the first time that Nanog mRNA expression can be detected with high sensitivity and specificity in lung cancer tissues. In addition, experiments on siRNA revealed that the constitutive expression of Nanog in cancer cells maintains proliferation ability; this is consistent with the observation that the overexpression of the Nanog gene promotes tumour cell growth (11). With regard to the expression of Nanog in cancers, Ezeh et al showed that the Nanog protein is expressed in tissues that were obtained from 2 breast cancer patients (12).…”

Section: Discussionsupporting

confidence: 60%

Diagnostic relevance of overexpressed Nanog gene in early lung cancers

Nirasawa

Kobayashi²,

Tsuji³

et al. 2009

Oncol Rep

View full text Add to dashboard Cite

Abstract. Currently, no target molecules have been identified that enable the diagnosis of lung cancer with high sensitivity and specificity, especially in the early clinical stages of cancer. Recently, Nanog has been reported to play an important role in the self-renewal and regeneration of ES cells by maintaining these cells in the undifferentiated state and by accelerating cell proliferation. Here, we compared the degree of Nanog mRNA expression in lung cancer tissues with that in non-cancerous tissues. Nanog mRNA was detected in 84.8% (39/46) of lung cancer tissues. The sensitivity and specificity of this diagnostic technique was 80.4 and 93.3%, respectively, as estimated using the cut-off obtained from the analysis of the receiver operating characteristic curve. Further, comparison of paired cancerous and non-cancerous tissues from the same patient revealed elevated Nanog mRNA levels in all patients. No obvious correlations were detected between the clinicopathological factors and Nanog mRNA expression; however, Nanog mRNA was expressed at high levels even in the early clinical stages of the cancer. In addition, the transduction of Nanog siRNA in lung carcinoma cells resulted in growth inhibition. These results suggest that Nanog mRNA might be a new tool to support the diagnosis of lung cancers, irrespective of the clinical stage.

show abstract

Section: Discussionsupporting

confidence: 60%

Diagnostic relevance of overexpressed Nanog gene in early lung cancers

Nirasawa

Kobayashi²,

Tsuji³

et al. 2009

Oncol Rep

View full text Add to dashboard Cite

show abstract

“…HA-CD44 interaction was proved to activate Nanog which is principally [20] involved in the stem cell maintenance and self-renewal in the ES cells [21,22]. The activation of CD44 through the PKCε phosphorylates Nanog, with or without the association of Stat3 regulates the expression of other pluripotent, tumorigenic and multidrug resistance genes [21]. Nanog has shown to regulate the expression of Sox2, Oct3/4, and Rex1, the prominent pluripotent transcription factors during embryonic stem cell pluripotency.…”

Section: Ha Induces the Expression Of Pluripotent Genesmentioning

confidence: 99%

“…These transcription factors are found to be over-expressed in several of the cancers and were used to identify cancer stem cell-like cells in glioblastoma [19]. HA-CD44 interaction was proved to activate Nanog which is principally [20] involved in the stem cell maintenance and self-renewal in the ES cells [21,22]. The activation of CD44 through the PKCε phosphorylates Nanog, with or without the association of Stat3 regulates the expression of other pluripotent, tumorigenic and multidrug resistance genes [21].…”

Section: Ha Induces the Expression Of Pluripotent Genesmentioning

confidence: 99%

Hyaluronic Acid Mediated Enrichment of CD44 Expressing Glioblastoma Stem Cells in U251MG Xenograft Mouse Model

Vaidyanath¹,

Mahmud²,

Khayrani³

et al. 2017

J Stem Cell Res Ther

View full text Add to dashboard Cite

“…Specifically, HA binding to CD44 is capable of stimulating MDR1 expression and drug resistance in breast tumour cells through ErbB2 signalling and PI3 kinase/Akt-related survival pathways (Misra et al, 2005). Bourguignon et al (2008) have recently shown that HA -CD44 interaction activates stem cell marker Nanog, Stat-3-mediated MDR1 gene expression and ankyrin-regulated multidrug efflux in breast and ovarian tumour cells. However, a direct link of phenotypes between drug resistance and invasion or metastasis in epithelial ovarian cancer (EOC) is still unclear.…”

mentioning

confidence: 99%

Coexpression of invasive markers (uPA, CD44) and multiple drug-resistance proteins (MDR1, MRP2) is correlated with epithelial ovarian cancer progression

et al. 2009

View full text Add to dashboard Cite

BACKGROUND: Invasion and metastases of cancer cells and the development of resistance to anticancer therapies are the main causes of treatment failure and mortality in cancer patients. METHODS: We evaluated invasive markers of urokinase plasminogen activator (uPA) and CD44 and multiple drug-resistance (MDR) markers of MDR1 and MRP2 in four epithelial ovarian cancer (EOC) cell lines, primary tumours (n ¼ 120) and matched metastatic lesions (n ¼ 40) by immunofluoresence labelling. We correlated uPA and CD44 with MDR markers in primary and metastatic cells using confocal microscope. We also investigated the relationship of the expression of uPA, CD44 and MDR1 with various progression parameters. RESULTS: The coexpression of uPA and CD44 with MDR markers was found in primary and metastatic cells. The overexpression of uPA, CD44 and MDR1 was found in most primary and matched metastatic lesions of EOC, and was significantly associated with tumour stage, grade, residual disease status, relapse and presence of ascites (Po0.05), but not with histology type (P40.05). CONCLUSIONS: Our results suggest that the overexpression of uPA, CD44 and MRD1 is correlated with EOC progression; both uPA and CD44 are related with drug resistance during EOC metastasis and could be useful therapeutically.

show abstract

Hyaluronan-CD44 Interaction Activates Stem Cell Marker Nanog, Stat-3-mediated MDR1 Gene Expression, and Ankyrin-regulated Multidrug Efflux in Breast and Ovarian Tumor Cells

Cited by 398 publications

References 97 publications

Diagnostic relevance of overexpressed Nanog gene in early lung cancers

Diagnostic relevance of overexpressed Nanog gene in early lung cancers

Hyaluronic Acid Mediated Enrichment of CD44 Expressing Glioblastoma Stem Cells in U251MG Xenograft Mouse Model

Coexpression of invasive markers (uPA, CD44) and multiple drug-resistance proteins (MDR1, MRP2) is correlated with epithelial ovarian cancer progression

Contact Info

Product

Resources

About