Synergism of EGFR and c-Met pathways, cross-talk and inhibition, in non-small cell lung cancer

Puri, Neelu; Salgia, Ravi

doi:10.4103/1477-3163.44372

Cited by 183 publications

(153 citation statements)

References 36 publications

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“…These preclinical studies suggested that the combination of inhibitors for MET and EGFR RTKs could potentially produce synergistic antitumor effects (24). Indeed, a synergistic effect on inhibition of cell proliferation and apoptosis was seen when a novel first-generation MET inhibitor, SU11274, was combined with EGFR inhibitors such as AG1478 or gefitinib (24). The synergism and cross-talk of EGFR and MET pathways in NSCLC, and the potential of simultaneous inhibition, were thus recognized in these studies.…”

Section: Hfg/met In Lung Cancermentioning

confidence: 88%

“…Indeed, synergistic effects of epidermal growth factor (EGF) and HGF on proliferation, and additive effects on motility, were noted in preclinical studies in NSCLC cells. For example, increased membrane ruffling to form a motile cell surface was observed when cells were stimulated with HGF and EGF independently, and when these growth factors were combined, an additive effect was observed (24). These preclinical studies suggested that the combination of inhibitors for MET and EGFR RTKs could potentially produce synergistic antitumor effects (24).…”

Section: Hfg/met In Lung Cancermentioning

confidence: 99%

“…For example, increased membrane ruffling to form a motile cell surface was observed when cells were stimulated with HGF and EGF independently, and when these growth factors were combined, an additive effect was observed (24). These preclinical studies suggested that the combination of inhibitors for MET and EGFR RTKs could potentially produce synergistic antitumor effects (24). Indeed, a synergistic effect on inhibition of cell proliferation and apoptosis was seen when a novel first-generation MET inhibitor, SU11274, was combined with EGFR inhibitors such as AG1478 or gefitinib (24).…”

Section: Hfg/met In Lung Cancermentioning

confidence: 99%

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MET in Lung Cancer: Biomarker Selection Based on Scientific Rationale

Salgia

2017

Molecular Cancer Therapeutics

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124

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MET or hepatocyte growth factor (HGF) receptor pathway signaling mediates wound healing and hepatic regeneration, with pivotal roles in embryonic, neuronal, and muscle development. However, dysregulation of MET signaling mediates proliferation, apoptosis, and migration and is implicated in a number of malignancies. In non-small cell lung cancer (NSCLC), aberrant MET signaling can occur through a number of mechanisms that collectively represent a significant proportion of patients. These include MET or HGF protein overexpression, MET gene amplification, MET gene mutation or fusion/rearrangement, or aberrations in downstream signaling or regulatory components. Responses to MET tyrosine kinase inhibitors have been documented in clinical trials in patients with MET-amplified or METoverexpressing NSCLC, and case studies or case series have shown that MET mutation/deletion is a biomarker that is also predictive of response to these agents. However, other recent clinical data have highlighted an urgent need to elucidate optimal biomarkers based on genetic and/or protein diagnostics to correctly identify patients most likely to benefit in ongoing clinical trials of an array of MET-targeted therapies of differing class. The latest advances in the development of MET biomarkers in NSCLC have been reviewed, toward establishing appropriate MET biomarker selection based on a scientific rationale. Mol Cancer Ther; 16(4); 555-65.Ó2017 AACR.

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Section: Hfg/met In Lung Cancermentioning

confidence: 88%

Section: Hfg/met In Lung Cancermentioning

confidence: 99%

Section: Hfg/met In Lung Cancermentioning

confidence: 99%

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MET in Lung Cancer: Biomarker Selection Based on Scientific Rationale

Salgia

2017

Molecular Cancer Therapeutics

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124

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“…The activated receptors such as VEGFR, EGFR, and c-Met play very important roles in the proliferation of cancer cells including lung cancer cells (Colon et al 2009;Kim et al 2008;Morelli et al 2006;Naumov et al 2009;Puri and Salgia 2008). In order to clarify the bufalin-targeted receptors in A549 cells, we studied the effects of bufalin on the related receptor phosphorylation and expressions in A549 cells.…”

Section: Bufalin Reduces the Receptor Phosphorylation And/or Protein mentioning

confidence: 99%

“…Suppression of the activated EGFR and ERK1/2 and p38 MAPKs as well as Akt signaling pathways led to inhibition of the proliferation of A549 cells (Baldys et al 2007;Nguyen et al 2004;Recchia et al 2009;Su et al 2010). There has been the cross-talk in EGFR and c-Met pathways in A549 cells which is related to the A549 cell proliferation (Puri and Salgia 2008). Suppression of EGFR, VEGFR, and c-Met led to inhibition of A549 cell proliferation in vitro and in vivo (Colon et al 2009;Kim et al 2008;Morelli et al 2006;Naumov et al 2009).…”

Section: Bufalin Reduces the Receptor Phosphorylation And/or Protein mentioning

confidence: 99%

Effects of bufalin on the proliferation of human lung cancer cells and its molecular mechanisms of action

et al. 2010

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Bufalin, a naturally occurring small-molecule compound from Traditional Chinese Medicine (TCM) Chansu showed inhibitory effects against human prostate, hepatocellular, endometrial and ovarian cancer cells, and leukemia cells. However, whether or not bufalin has inhibitory activity against the proliferation of human non-small cell lung cancer (NSCLC) cells is unclear. The aim of this study is to study the effects of bufalin on the proliferation of NSCLC and its molecular mechanisms of action. The cancer cell proliferation was measured by MTT assay. The apoptosis and cell cycle distribution were analyzed by flow cytometry. The protein expressions and phosphorylation in the cancer cells were detected by Western blot analysis. In the present study, we have demonstrated that bufalin suppressed the proliferation of human NSCLC A549 cell line in time-and dosedependent manners. Bufalin induced the apoptosis and cell cycle arrest by affecting the protein expressions of Bcl-2/Bax, cytochrome c, caspase-3, PARP, p53, p21WAF1, cyclinD1, and COX-2 in A549 cells. In addition, bufalin reduced the protein levels of receptor expressions and/or phosphorylation of VEGFR1, VEGFR2, EGFR and/or c-Met in A549 cells. Furthermore, bufalin inhibited the protein expressions and phosphorylation of Akt, NF-jB, p44/42 MAPK (ERK1/2) and p38 MAPK in A549 cells. Our results suggest that bufalin inhibits the human lung cancer cell proliferation via VEGFR1/VEGFR2/EGFR/cMet-Akt/p44/42/p38-NF-jB signaling pathways; bufalin may have a wide therapeutic and/or adjuvant therapeutic application in the treatment of human NSCLC.

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