Kinase-Dead BRAF and Oncogenic RAS Cooperate to Drive Tumor Progression through CRAF

Heidorn, Sonja J.; Milagre, Carla; Whittaker, Steven R.; Nourry, Arnaud; Niculescu-Duvas, Ion; Dhomen, Nathalie; Hussain, Jahan; Reis‐Filho, Jorge S.; Springer, Caroline J.; Pritchard, Catrin; Marais, Richard

doi:10.1016/j.cell.2009.12.040

Cited by 1,314 publications

(1,359 citation statements)

References 34 publications

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“…For example, the finding that approximately 50% of melanomas harbour oncogenic BRAF mutations has driven drug discovery programmes that have generated potent, selective inhibitors that are active against V600E BRAF mutant tumor cells (25)(26)(27). These agents have yielded dramatic results in clinical trials in patients with V600E BRAF mutant melanoma (28,29).…”

Section: Discussionmentioning

confidence: 99%

“…These observations highlight the need for continued research effort in to novel therapies for BRAF mutant melanoma. As a note of caution, however, the importance of a detailed understanding of the molecular pathology of MMM was underlined in preclinical work that showed that, in BRAF wild-type tumor cells, the use of a BRAF inhibitor can activate signalling through BRAF-CRAF dimerisation and, as a result, may accelerate tumor growth (27). Therefore, future development of specific targeted therapies for MMM must include a detailed analysis of the various genetic backgrounds of this disease.…”

Section: Discussionmentioning

confidence: 99%

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Synergistic cytotoxicity of radiation and oncolytic Lister strain vaccinia in V600D/EBRAF mutant melanoma depends on JNK and TNF-α signaling

Khan

Mansfield

et al. 2013

Oncogene

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Melanoma is an aggressive skin cancer that carries an extremely poor prognosis when local invasion, nodal spread or systemic metastasis has occurred. Recent advances in melanoma biology have revealed that RAS-RAF-MEK-ERK signalling plays a pivotal role in governing disease progression and treatment resistance. Proof-of-concept clinical studies have shown that direct BRAF inhibition yields impressive responses in advanced disease but these are short-lived as treatment resistance rapidly emerges. Therefore, there is a pressing need to develop new targeted strategies for BRAF mutant melanoma.As such, oncolytic viruses represent a promising cancer-specific approach with significant activity in melanoma.This study investigated interactions between genetically-modified vaccinia virus (GLV1h68) and radiotherapy in melanoma cell lines with BRAF mutant, Ras mutant or wildtype genotype. Pre-clinical studies revealed that GLV-1h68 combined with radiotherapy significantly increased cytotoxicity and apoptosis relative to either single agent in V600D BRAF/ V600E BRAF mutant melanoma in vitro and in vivo. The mechanism of enhanced cytotoxicity with GLV-1h68/radiation was independent of viral replication and due to attenuation of JNK, p38 and ERK MAPK phosphorylation specifically in BRAF mutant cells. Further studies showed that JNK pathway inhibition sensitized BRAF mutant cells to GLV-1h68-mediated cell death, mimicking the effect of radiation. GLV1h68 infection activated MAPK signalling in V600D BRAF/ V600E BRAF mutant cell lines and this was associated with TNF-α secretion which, in turn, provided a prosurvival signal.Combination GLV-1h68/radiation (or GLV-1h68/JNK inhibition) caused abrogation of TNF-α secretion. These data provide a strong rationale for combining GLV-1h68 with irradiation in V600D/E BRAF mutant tumors.3

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Synergistic cytotoxicity of radiation and oncolytic Lister strain vaccinia in V600D/EBRAF mutant melanoma depends on JNK and TNF-α signaling

Khan

Mansfield

et al. 2013

Oncogene

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“…This work was essential in identifying MEK as being of particular importance in BRAF-inhibitor resistance and, thus, the potential synergy between BRAF and MEK inhibitors 55 . The mechanistic specificity of this work additionally led to the description of a phenomenon dubbed 'paradoxical activation' of the MAPK pathway via BRAF inhibition in BRAF-wild-type cells, for example, keratinocytes [56][57][58][59] . This discovery suggested that some of the hyperproliferative cutaneous manifestations associated with BRAF inhibition in the clinic might be mitigated by combination therapy incorporating a MEK inhibitor.…”

Section: Braf-targeted Therapiesmentioning

confidence: 99%

Targeted agents and immunotherapies: optimizing outcomes in melanoma

et al. 2017

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“…Furthermore, as this inhibitor is only effective on cells transformed by this V600E mutation, another BRaf-specific inhibitor, GSK2118436, which targets the V600K mutation, is also in a small phase III trial having shown great potential in patients with brain metastases 81 . However some caution remains as the inhibition of the BRaf mutation V600E (and also V600K by GSK2118436) with these BRaf inhibitors has been shown in some patients to reactivate the MAPK pathway through CRaf 82,83 , and developing resistance to BRaf inhibitors is a problem.…”

Section: Current Therapies In the Treatment Of Metastatic Melanomamentioning

confidence: 99%

Role of the pro-survival molecule Bfl-1 in melanoma

Hind

Carter

Harris

et al. 2015

The International Journal of Biochemistry & Cell Biology

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Melanoma, the cancer derived from the melanocytes of the skin, is becoming an ever more common cancer in the ageing population of the developed world and displays an intrinsic resistance to current therapies. This chemo resistance makes metastatic melanoma an extremely difficult cancer to treat leading to a 5 year survival rate of just 20%. As such, it is important to unearth new potential drug targets to increase the prospects for melanoma patients.Bfl-1 is a pro-survival protein of the Bcl-2 family of apoptosis regulating proteins. It has been found to be over-expressed in a small subset of chemo resistant tumours, including melanoma. Accordingly, I characterised the molecule in melanoma cells and determined its role in protecting these cells from chemotherapy-induced apoptosis. I elucidated the expression profile and half-lives of the protein and mRNA across a panel of melanoma cell-lines and healthy melanocytes. I also confirmed, using pathway specific inhibitors, that Bfl-1 was transcriptionally regulated by the NFB pathway and concluded through pulsechase experiments that Bfl-1 protein was degraded, at least in part, by the proteasome. Subcellular fractionation and indirect immunofluorescence techniques elucidated that Bfl-1 was located mostly at the mitochondria in both resting and apoptotic cells, with a diffuse level present throughout the cytoplasm. As well as characterising the protein in both melanoma cells and healthy primary melanocytes, I determined its role in the resistance of these cells to apoptosis. Over-expressed Bfl-1 was found to protect melanoma cells from apoptosis caused by a range of chemotherapeutic agents in A375 melanoma cells, which naturally expressed very low levels of Bfl-1. Further, knock down of Bfl-1 using siRNA technology in melanoma cells revealed the dependence of these cells on Bfl-1 for their resistance to certain chemotherapeutic agents currently used in melanoma treatment, including the MEK inhibitor PD901. All together, this research contributes to our understanding of Bfl-1 and highlights it as a potentially important therapeutic target in metastatic melanoma.

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Kinase-Dead BRAF and Oncogenic RAS Cooperate to Drive Tumor Progression through CRAF

Cited by 1,314 publications

References 34 publications

Synergistic cytotoxicity of radiation and oncolytic Lister strain vaccinia in V600D/EBRAF mutant melanoma depends on JNK and TNF-α signaling

Synergistic cytotoxicity of radiation and oncolytic Lister strain vaccinia in V600D/EBRAF mutant melanoma depends on JNK and TNF-α signaling

Targeted agents and immunotherapies: optimizing outcomes in melanoma

Role of the pro-survival molecule Bfl-1 in melanoma

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