Phase I Expansion and Pharmacodynamic Study of the Oral MEK Inhibitor RO4987655 (CH4987655) in Selected Patients with Advanced Cancer with <i>RAS–RAF</i> Mutations

Zimmer, Lisa; Barlési, Fabrice; Martinez-García, Maria; Dièras, Véronique; Schellens, Jan H.M.; Spano, Jean‐Philippe; Middleton, Mark R.; Calvo, Emiliano; Paz-Ares, L.; Larkin, James; Pacey, Simon; Venturi, Miro; Kraeber-Bodéré, Françoise; Tessier, Jean; Eberhardt, Wilfried; Pâques, M.; Guarin, Ernesto; Méresse, Valérie; Soria, Jean‐Charles

doi:10.1158/1078-0432.ccr-14-0341

Cited by 65 publications

(50 citation statements)

References 49 publications

(61 reference statements)

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“…Toxicities observed with RO4987655 have been similar to those described with other MEK inhibitors [113]. Common toxicities have included those that were skin related (rash and acneiform dermatitis), gastrointestinal disorders (nausea, vomiting, diarrhea), ocular (serous retinal detachment and blurred vision), and general (peripheral edema and asthenia).…”

Section: Safetymentioning

confidence: 66%

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The Biology and Clinical Development of MEK Inhibitors for Cancer

Luke

Ott

Shapiro

2014

Drugs

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The mitogen-activated protein kinase kinases (MAPKK) MEK1 and MEK2 are integral members of the MAPK/ERK signaling pathway and are of interest in the development of anti-cancer therapeutics. The MAPK/ERK pathway is dysregulated in more than 30 % of cancers, predominately by mutations in RAS and BRAF proteins, and MEK serves as a potential downstream target for both of these. The biology of MEK inhibition is complex, as the molecule is differentially regulated by upstream RAS or RAF. This has impacted on the past development of MEK inhibitors as treatments for cancer and may be exploited in more rational, molecularly selected drug development plans in the future. The role of MEK in cancer and the mechanism of action of MEK inhibitors is reviewed. Furthermore, MEK inhibitors that are available in standard practice, as well as those most advanced in clinical development, are discussed. Finally, next steps in the development of MEK inhibitors are considered.

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Section: Safetymentioning

confidence: 66%

“…RO4987655 has been evaluated in several expansion arms of the phase I dose-escalation study including melanoma, NSCLC, and colorectal carcinoma [113]. Among patients with melanoma, four of 18 (24 %) BRAF mutant and four of 20 (20 %) BRAF WT had a response, with PR as best response in these cohorts.…”

Section: Clinical Activitymentioning

confidence: 99%

The Biology and Clinical Development of MEK Inhibitors for Cancer

Luke

Ott

Shapiro

2014

Drugs

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“…Other studies are currently ongoing in several types of solid malignancies [72][73][74][75][76][77][78][79][80][81][82][83]. The maximum tolerated dose recommended as a single agent is 100 mg per day, given orally as either 50 mg bid or 100 mg qd (every day).…”

Section: Growth Factorsmentioning

confidence: 99%

MEK 1/2 inhibitors in the treatment of hepatocellular carcinoma

Facciorusso

Licinio

Carr

et al. 2015

Expert Review of Gastroenterology & Hepatology

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Sorafenib is the only approved systemic treatment for advanced hepatocellular carcinoma patients and all the recently published randomized controlled trials on new systemic drugs have been unsuccessful. This is likely due to a lack of understanding of tumor progression, molecular drivers, and liver toxicity, as well as flaws in trial design. An important signaling pathway in hepatocarcinogenesis is the MEK cascade involved in various cellular responses, including adaptation and survival. A key role in this cascade is played by MEK, of which MEK 1/2 represent the prototypes and an interesting target for new oncological drugs. This review analyzes recent developments and future perspectives on the role of MEK inhibitors in hepatocellular carcinoma treatment.

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“…RO5126766 binds MEK and suppresses the phosphorylation of MEK by Raf via the formation of a stable Raf:MEK complex. Phase I/II studies of those allosteric modulators in patients with advanced solid tumors were performed [77][78][79][80], while the efficacy and potential mechanisms of those inhibitors against lung cancer need to be furthermore explored.…”

Section: Allosteric Inhibitors For Lung Cancermentioning

confidence: 99%

Allosteric therapies for lung cancer

Jing

Wang

2015

Cancer Metastasis Rev

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Allostery is a regulation at a distance by conveying information from one site to another and an intrinsic property of dynamic proteins. Allostery plays an essential role in receptor trafficking, signal transmission, controlled catalysis, gene turn on/off, or cell apoptosis. Allosteric mutations are considered as one of causes responsible for cancer development, leading to "allosteric diseases" by stabilizing an active or inactive conformation or changing the dynamic distribution of preexisting propagation pathways. The present article mainly focuses on the potential of allosteric therapies for lung cancer. Allosteric drugs may have several advantages over traditional drugs. The epidermal growth factor receptor mutations and signaling pathways downstream (such as PI3K/AKT/mTOR and RAS/RAF/MEK/ERK pathways) were suggested to play a key role in lung cancer and considered as targets of allosteric therapy. Some allosteric inhibitors for lung cancer-specific targets and a series of preclinical trials of allosteric inhibitors for lung cancer have been developed and reported. We expect that allosteric therapies will gain more attentions to develop combinatorial strategies for lung cancer and metastasis.

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Phase I Expansion and Pharmacodynamic Study of the Oral MEK Inhibitor RO4987655 (CH4987655) in Selected Patients with Advanced Cancer with RAS–RAF Mutations

Cited by 65 publications

References 49 publications

The Biology and Clinical Development of MEK Inhibitors for Cancer

The Biology and Clinical Development of MEK Inhibitors for Cancer

MEK 1/2 inhibitors in the treatment of hepatocellular carcinoma

Allosteric therapies for lung cancer

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