Molecular alterations associated with acquired resistance to BRAFV600E targeted therapy in melanoma cells

Szász, István; Koroknai, Viktória; Kiss, Tímea; Vízkeleti, Laura; Ádány, Róza; Balázs, Margit

doi:10.1097/cmr.0000000000000588

Cited by 15 publications

(31 citation statements)

References 47 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Overexpressed genes in BRAF inhibitor-resistant cells are often associated with growth factors and their receptors, cell adhesion molecules and extracellular matrix binding [ 84 ]. Common mutations involve effects on receptor tyrosine kinases (RTKs), such as epidermal growth factor receptor (EGFR), platelet-derived growth factor receptor (PDGFR), hepatocyte growth factor (HGF), or insulin-like growth factor (IGF) receptor, which in turn activate parallel pathways [ 11 , 19 , 20 , 25 , 29 , 58 , 59 , 84 , 85 , 86 ]. Research has shown extensive redundancy in RTK-mediated signaling pathways, whereby a broad range of widely expressed RTKs are upregulated in cells with BRAF inhibitor resistance [ 86 ].…”

Section: Resultsmentioning

confidence: 99%

Mechanisms of Acquired BRAF Inhibitor Resistance in Melanoma: A Systematic Review

Proietti

Skroza

Bernardini

et al. 2020

Cancers

View full text Add to dashboard Cite

This systematic review investigated the literature on acquired v-raf murine sarcoma viral oncogene homolog B1 (BRAF) inhibitor resistance in patients with melanoma. We searched MEDLINE for articles on BRAF inhibitor resistance in patients with melanoma published since January 2010 in the following areas: (1) genetic basis of resistance; (2) epigenetic and transcriptomic mechanisms; (3) influence of the immune system on resistance development; and (4) combination therapy to overcome resistance. Common resistance mutations in melanoma are BRAF splice variants, BRAF amplification, neuroblastoma RAS viral oncogene homolog (NRAS) mutations and mitogen-activated protein kinase kinase 1/2 (MEK1/2) mutations. Genetic and epigenetic changes reactivate previously blocked mitogen-activated protein kinase (MAPK) pathways, activate alternative signaling pathways, and cause epithelial-to-mesenchymal transition. Once BRAF inhibitor resistance develops, the tumor microenvironment reverts to a low immunogenic state secondary to the induction of programmed cell death ligand-1. Combining a BRAF inhibitor with a MEK inhibitor delays resistance development and increases duration of response. Multiple other combinations based on known mechanisms of resistance are being investigated. BRAF inhibitor-resistant cells develop a range of ‘escape routes’, so multiple different treatment targets will probably be required to overcome resistance. In the future, it may be possible to personalize combination therapy towards the specific resistance pathway in individual patients.

show abstract

Section: Resultsmentioning

confidence: 99%

Mechanisms of Acquired BRAF Inhibitor Resistance in Melanoma: A Systematic Review

Proietti

Skroza

Bernardini

et al. 2020

Cancers

View full text Add to dashboard Cite

show abstract

“…Development of acquired resistance after initial response leads to tumour regrowth [24]. Both genetic and epigenetic alterations are involved in the development of acquired resistance [2].…”

Section: Discussionmentioning

confidence: 99%

“…Resistant cell lines were established as described before, by continuously increasing the concentration of Vemurafenib analogue PLX4720 with every passage for 3 months [24]. In brief, WM983A, WM983B cell lines were seeded at low densities in T25 flasks until cell confluence reached about 80%.…”

Section: Establishment Of Braf Inhibitor Resistant Cell Linesmentioning

confidence: 99%

Gene Expression Signature of BRAF Inhibitor Resistant Melanoma Spheroids

Koroknai

Patel

Szász

et al. 2020

Pathol. Oncol. Res.

Self Cite

View full text Add to dashboard Cite

In vitro cell cultures are frequently used to define the molecular background of drug resistance. The majority of currently available data have been obtained from 2D in vitro cultures, however, 3D cell culture systems (spheroids) are more likely to behave similarly to in vivo conditions. Our major aim was to compare the gene expression signature of 2D and 3D cultured BRAFV600E mutant melanoma cell lines. We successfully developed BRAF-drug resistant cell lines from paired primary/ metastatic melanoma cell lines in both 2D and 3D in vitro cultures. Using Affymetrix Human Gene 1.0 ST arrays, we determined the gene expression pattern of all cell lines. Our analysis revealed 1049 genes (562 upregulated and 487 downregulated) that were differentially expressed between drug-sensitive cells grown under different cell cultures. Pathway analysis showed that the differently expressed genes were mainly associated with the cell cycle, p53, and other cancer-related pathways. The number of upregulated genes (72 genes) was remarkably fewer when comparing the resistant adherent cells to cells that grow in 3D, and were associated with cell adhesion molecules and IGF1R signalling. Only 1% of the upregulated and 5.6% of the downregulated genes were commonly altered between the sensitive and the resistant spheroids. Interestingly, we found several genes (BNIP3, RING1 and ABHD4) with inverse expression signature between sensitive and resistant spheroids, which are involved in anoikis resistance and cell cycle regulation. In summary, our study highlights gene expression alterations that might help to understand the development of acquired resistance in melanoma cells in tumour tissue.

show abstract

“…This triggers then constant proliferation in melanoma cells, leading to melanoma and treatable well by by a combination of B-Raf and MEK inhibitors (e.g., vemurafenib and cobimetanib). However, resistance is an issue of the treatment with these inhibitors and additional therapeutic options are necessary such as ERK1/2 inhibitors or alternative targeting strategies of protein kinases [10,11].…”

Section: Introductionmentioning

confidence: 99%

“…Moreover, it describes and models all nodes of the whole network considered and this for all time points and all desired pharmacological interventions. Nevertheless, for each real situation, comparison and validation by experimental data is critical and also here the ERK cascade is a nice and well-studied example (e.g., [7,8,9,10,11,14]).…”

Section: Introductionmentioning

confidence: 99%

How to Steer and Control ERK and the ERK Signaling Cascade Exemplified by Looking at Cardiac Insufficiency

Breitenbach

Lorenz

Dandekar

2019

IJMS

View full text Add to dashboard Cite

Mathematical optimization framework allows the identification of certain nodes within a signaling network. In this work, we analyzed the complex extracellular-signal-regulated kinase 1 and 2 (ERK1/2) cascade in cardiomyocytes using the framework to find efficient adjustment screws for this cascade that is important for cardiomyocyte survival and maladaptive heart muscle growth. We modeled optimal pharmacological intervention points that are beneficial for the heart, but avoid the occurrence of a maladaptive ERK1/2 modification, the autophosphorylation of ERK at threonine 188 (ERK Thr 188 phosphorylation), which causes cardiac hypertrophy. For this purpose, a network of a cardiomyocyte that was fitted to experimental data was equipped with external stimuli that model the pharmacological intervention points. Specifically, two situations were considered. In the first one, the cardiomyocyte was driven to a desired expression level with different treatment strategies. These strategies were quantified with respect to beneficial effects and maleficent side effects and then which one is the best treatment strategy was evaluated. In the second situation, it was shown how to model constitutively activated pathways and how to identify drug targets to obtain a desired activity level that is associated with a healthy state and in contrast to the maleficent expression pattern caused by the constitutively activated pathway. An implementation of the algorithms used for the calculations is also presented in this paper, which simplifies the application of the presented framework for drug targeting, optimal drug combinations and the systematic and automatic search for pharmacological intervention points. The codes were designed such that they can be combined with any mathematical model given by ordinary differential equations.

show abstract

Molecular alterations associated with acquired resistance to BRAFV600E targeted therapy in melanoma cells

Cited by 15 publications

References 47 publications

Mechanisms of Acquired BRAF Inhibitor Resistance in Melanoma: A Systematic Review

Mechanisms of Acquired BRAF Inhibitor Resistance in Melanoma: A Systematic Review

Gene Expression Signature of BRAF Inhibitor Resistant Melanoma Spheroids

How to Steer and Control ERK and the ERK Signaling Cascade Exemplified by Looking at Cardiac Insufficiency

Contact Info

Product

Resources

About