c-Met Overexpression Is a Prognostic Factor in Ovarian Cancer and an Effective Target for Inhibition of Peritoneal Dissemination and Invasion

Sawada, Kenjiro; Radjabi, A. Reza; Shinomiya, Nariyoshi; Kistner, Emily O.; Kenny, Hilary A.; Becker, Amy R.; Turkyilmaz, Muge; Salgia, Ravi; Yamada, S. Diane; Woude, George F. Vande; Tretiakova, Maria; Lengyel, Ernst

doi:10.1158/0008-5472.can-06-1147

Cited by 242 publications

(269 citation statements)

References 38 publications

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“…To test this, we examined a set of inhibitors at effective concentrations that specifically inhibit various RTKs, including general RTKs (genistein), IGF-1R (AG1024), fibroblast growth factor receptor 1 (SU5402), epidermal growth factor receptor (EGFR) (AG1478) and hepatocyte growth factor receptor c-Met (K252a), which have been previously implicated in the progression and metastasis of ovarian cancer (Ellerbroek et al, 2001;Steele et al, 2001;Brokaw et al, 2007;Sawada et al, 2007). Among these inhibitors, we found that only genistein used to block RTK or AG1024 used to inhibit IGF-1R led to a marked decrease in p120 ctn activation ( Figure 3a) and translocation ( Figure 3b) following GnRHa stimulation.…”

Section: Resultsmentioning

confidence: 99%

P-cadherin cooperates with insulin-like growth factor-1 receptor to promote metastatic signaling of gonadotropin-releasing hormone in ovarian cancer via p120 catenin

et al. 2011

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Gonadotropin-releasing hormone (GnRH) is a potent prometastatic factor in ovarian cancer, but the intracellular signaling events are not well understood. The classical Ga q -phospholipase C signal transduction pathway known to operate in the pituitary is not involved in GnRH actions at non-pituitary targets. Here we showed that GnRH treatment of ovarian cancer cells led to a rapid and remarkable tyrosine phosphorylation of p120 catenin (p120 ctn ), which was mediated by P-cadherin. The use of P-cadherin small interfering RNA or neutralizing antibodies to inhibit P-cadherin expression and function resulted in diminished p120 ctn activation, confirming that the effect was P-cadherin specific. On exploring how P-cadherin, which lacks intrinsic kinase activity, might regulate the activation of p120 ctn , we found that P-cadherin could induce the ligandindependent activation of insulin-like growth factor-1 receptor (IGF-1R). Inhibition of IGF-1R expression or its activity significantly inhibited GnRH-induced p120 ctn activation, and the subsequent cell migration and invasion. In addition, we showed that IGF-1R regulation by P-cadherin was associated with complex formation between IGF-1R and P-cadherin, and this regulation was also observed to be in vivo correlated with metastasis. Furthermore, using a mouse model of ovarian cancer metastasis, GnRH receptor knockdown was shown to diminish peritoneal dissemination of tumors and ascites formation. These findings suggest for the first time that GnRH can initiate an outside-in p120 ctn signal transduction through the cross-talk between P-cadherin and IGF-1R, thus providing a novel molecular mechanism by which GnRH may control the high level of aggressiveness and invasion and metastasis potential that are characteristic of ovarian cancer.

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Section: Resultsmentioning

confidence: 99%

P-cadherin cooperates with insulin-like growth factor-1 receptor to promote metastatic signaling of gonadotropin-releasing hormone in ovarian cancer via p120 catenin

et al. 2011

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“…In recent years, mis-regulation of the HGF/cMET pathway has been investigated in ovarian cancer, and high expression of cMET has been identified in subsets of all four major histotypes of EOC (high grade serous, clear cell, mucinous, and endometrioid [22][23][24][25][26][27][28][29]). It must be noted, however, that the outcome from this over-expression remains unclear.…”

Section: Hgf/cmet In Ovarian Cancermentioning

confidence: 99%

“…It must be noted, however, that the outcome from this over-expression remains unclear. While several studies have demonstrated a correlation between high cMET expression and poor prognosis [25,30], others have shown no statistically significant correlation between cMET expression and shorter survival [26,29], and still others suggest that cMET is expressed in early tumours, and is associated with good prognostic factors [23]. It should be noted that the majority of these studies were performed on relatively small numbers of samples, and usually contained mixed subtypes of EOC, thus further confusing the matter.…”

Section: Hgf/cmet In Ovarian Cancermentioning

confidence: 99%

“…For example, recent IHC studies performed on gastric tumour samples have reported cMET over-expression in 4-63% of cases [72][73][74][75][76][77] and various studies performed in ovarian cancer estimate high expression of cMET to be present in 11-68 % of cases [30,22,23,26,25] (Table 1). The majority of the estimates above come from IHC studies, using a number of different antibodies, but no consensus on scoring criteria yet exists, nor whether cytoplasmic or membranous staining for cMET is important.…”

Section: Ihc For Cmetmentioning

confidence: 99%

“…However, surprisingly, no biomarkers were used, nor were analyses performed post-hoc on patients responding to treatment. With current estimates of high cMET expression occurring in 11-68% of ovarian cancer cases (see Table 1) [30,22,23,26,25], it is possible that as few as 3 patients enrolled within the study were in a position to benefit from receiving the anti-HGF antibody, and that as many as 29 patients potentially to do worse upon receiving the therapy.…”

Section: Hgf/cmet Inhibitors Trials In Ovarian Cancermentioning

confidence: 99%

See 2 more Smart Citations

The Therapeutic Potential of Targeting the HGF/cMET Axis in Ovarian Cancer

Moran-Jones

2016

Mol Diagn Ther

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Survival rates for ovarian cancer have remained relatively stable for the past two decades, despite advances in surgical techniques and cytotoxic chemotherapeutics, indicating a requirement for better therapies. One pathway currently proposed for targeting is the HGF/cMET pathway. Up-regulated in a number of tumour types, cMET is a tyrosine kinase receptor expressed on epithelial cells. In ovarian cancer, it has been identified as highly expressed in the four major subtypes, with expression estimates ranging from 11-68% of cases. HGF, the only known ligand for cMET, is found at high levels in both serum and ascites in women with ovarian cancer, and proposed to induce both migration and metastasis. However, clinically validated biomarkers are not yet available for either HGF or cMET, preventing a clear understanding of the true rate of over-expression, or its correlation with prognosis.

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The levels of soluble cMET ectodomain in the blood of patients with ovarian cancer are an independent prognostic biomarker

et al. 2021

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cMET mesenchymal-epithelial transition tyrosine kinase sMET a soluble cMET ectodomain HR hazard ratio PFS progression-free survival OS overall survival TPR translocated promoter region HGF hepatocyte growth factor MMP9 matrix metalloprotease 9 EGFR-TKI epidermal growth factor receptor tyrosine kinase inhibitor NSCLC non small cell lung cancer FIGO Fédération Internationale de Gynécologie et d'Obstétrique CI confidence intervall AUC area under the curve ROC receiver operating characteristic ED estimated difference BMI body mass index ADAM a disintegrin and metalloprotease

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c-Met Overexpression Is a Prognostic Factor in Ovarian Cancer and an Effective Target for Inhibition of Peritoneal Dissemination and Invasion

Abstract: The hepatocyte growth factor receptor c-Met is a receptor tyrosine kinase that plays an important role in tumor growth by activating mitogenic signaling pathways.

Cited by 242 publications

References 38 publications

P-cadherin cooperates with insulin-like growth factor-1 receptor to promote metastatic signaling of gonadotropin-releasing hormone in ovarian cancer via p120 catenin

P-cadherin cooperates with insulin-like growth factor-1 receptor to promote metastatic signaling of gonadotropin-releasing hormone in ovarian cancer via p120 catenin

The Therapeutic Potential of Targeting the HGF/cMET Axis in Ovarian Cancer

The levels of soluble cMET ectodomain in the blood of patients with ovarian cancer are an independent prognostic biomarker

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