Expression and activity of EGFR in human cutaneous melanoma cell lines and influence of vemurafenib on the EGFR pathway

Groß, Alexander; Niemetz-Rahn, Annett; Nonnenmacher, Anika; Tucholski, Johannes; Keilholz, Ulrich; Fusi, Alberto

doi:10.1007/s11523-014-0318-9

Cited by 32 publications

(29 citation statements)

References 32 publications

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“…Our data is also consonant with a recent report that high EGFR expressing cells often lack EGFR activation, presumably due to lack of ligands, and are still sensitive to BRAFi; thus, EGFR levels alone cannot be used as a biomarker of vemurafenib resistance(Gross et al ., 2014). Our results also suggest that ligand measurement in blood or other body fluid might be an eventual method to predict drug resistance clinically.…”

Section: Discussionsupporting

confidence: 91%

MITF Modulates Therapeutic Resistance through EGFR Signaling

Chen

Kumar

et al. 2015

Journal of Investigative Dermatology

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Response to targeted therapies varies significantly despite shared oncogenic mutations. Nowhere is this more apparent than in BRAF(V600E)-mutated melanomas where initial drug response can be striking and yet relapse is commonplace. Resistance to BRAF inhibitors have been attributed to the activation of various receptor tyrosine kinases (RTKs) though the underlying mechanisms have been largely uncharacterized. Here, we found that EGFR induced vemurafenib resistance is ligand dependent. We then employed whole-genome expression analysis and discovererd that vemurafenib resistance correlated with the loss of MITF, along with its melanocyte lineage program, and with the activation of EGFR signaling. An inverse relationship between MITF, vemurafenib resistance and EGFR was then observed in patient samples of recurrent melanoma and was conserved across melanoma cell lines and patients’ tumor specimens. Functional studies revealed that MITF depletion activated EGFR signaling and consequently recapitulated the resistance phenotype. In contrast, forced expression of MITF in melanoma and colon cancer cells inhibited EGFR and conferred sensitivity to BRAF/MEK inhibitors. These findings indicate that an “autocrine drug resistance loop” is suppressed by melanocyte lineage signal(s), such as MITF. This resistance loop modulates drug response and could explain the unique sensitivity of melanomas to BRAF inhibition.

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Section: Discussionsupporting

confidence: 91%

MITF Modulates Therapeutic Resistance through EGFR Signaling

Chen

Kumar

et al. 2015

Journal of Investigative Dermatology

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“…We also showed that SKMEL-28 R cells resisted to vemurafenib via overexpression of EGFR, pTyrosine1173-EGFR, pThr308-AKT and pSer473-AKT. These results are in accordance with previous reports (Chen et al, 2012;Gross et al, 2014). Vemurafenib-induced pAKTs were inhibited by MK-2206, an AKT inhibitor or by paclitaxel or by combined MK-2206 and paclitaxel (Figure 5a).…”

Section: Discussionsupporting

confidence: 93%

“…Normally EGFR expression level in SKMEL-28 is quite low however it is overexpressed in acquired resistance to vemurafenib cells (Prahallad et al, 201;Gross et al, 2014). Therefore we decided to investigate the role of EGFR and phosphorylated EGFR (pEGFR) in regulating of pAKT.…”

Section: 699 Treatment Of Vemurafenib-resistant Skmel-28 Melanoma Cementioning

confidence: 99%

Treatment of Vemurafenib-Resistant SKMEL-28 Melanoma Cells with Paclitaxel

Thắng

Phan

Kumasaka

et al. 2015

Asian Pacific Journal of Cancer Prevention

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“…Increased ERK phosphorylation in wild-type BRAF melanoma cell lines has been observed, reducing cell adherence and increasing migration after vemurafenib treatment [107]. In SK-MEL-24 and MEL-HO cell lines, AKT phosphorylation increased after treatment with vemurafenib, while AKT activation decreased in SK-MEL-28, Colo800, and IPC298 BRAF wild-type cells [108]. One challenge associated with BRAF-targeted treatment is the tendency for melanoma to develop resistance to treatment.…”

Section: Effects Of Small Molecule Inhibitors On Emt In Melanomamentioning

confidence: 99%

Potential therapeutic targets of epithelial–mesenchymal transition in melanoma

et al. 2017

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Melanoma is a cutaneous neoplastic growth of melanocytes with great potential to invade and metastasize, especially when not treated early and effectively. Epithelial-mesenchymal transition (EMT) is the process by which melanocytes lose their epithelial characteristics and acquire mesenchymal phenotypes. Mesenchymal protein expression increases the motility, invasiveness, and metastatic potential of melanoma. Many pathways play a role in promotion of mesenchymal protein expression including RAS/RAF/MEK/ERK, PI3K/AKT/mTOR, Wnt/β-catenin, and several others. Downstream effectors of these pathways induce expression of EMT transcription factors including Snail, Slug, Twist, and Zeb that promote repression of epithelial and induction of mesenchymal character. Emerging research has demonstrated that a variety of small molecule inhibitors as well as phytochemicals can influence the progression of EMT and may even reverse the process, inducing re-expression of epithelial markers. Phytochemicals are of particular interest as supplementary treatment options because of their relatively low toxicities and anti-EMT properties. Modulation of EMT signaling pathways using synthetic small molecules and phytochemicals is a potential therapeutic strategy for reducing the aggressive progression of metastatic melanoma. In this review, we discuss the emerging pathways and transcription factor targets that regulate EMT and evaluate potential synthetic small molecules and naturally occurring compounds that may reduce metastatic melanoma progression.

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Expression and activity of EGFR in human cutaneous melanoma cell lines and influence of vemurafenib on the EGFR pathway

Cited by 32 publications

References 32 publications

MITF Modulates Therapeutic Resistance through EGFR Signaling

MITF Modulates Therapeutic Resistance through EGFR Signaling

Treatment of Vemurafenib-Resistant SKMEL-28 Melanoma Cells with Paclitaxel

Potential therapeutic targets of epithelial–mesenchymal transition in melanoma

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