Antitumor Efficacy of the Novel RAF Inhibitor GDC-0879 Is Predicted by BRAFV600E Mutational Status and Sustained Extracellular Signal-Regulated Kinase/Mitogen-Activated Protein Kinase Pathway Suppression

Hoeflich, Klaus P.; Herter, Sylvia; Tien, Janet; Wong, Leo Lap-Yan; Berry, Leanne; Chan, Jocelyn; O’Brien, Carol; Modrušan, Zora; Seshagiri, Somasekar; Lackner, Mark R.; Stern, Howard M.; Choo, Edna F.; Murray, Lesley J.; Friedman, Lori S.; Belvin, Marcia

doi:10.1158/0008-5472.can-08-3563

Cited by 160 publications

(115 citation statements)

References 25 publications

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“…Whether this development results from the induction of ERK signaling by PLX4032 is unknown. Others also have noted ERK activation in tumors with BRAF WT that have been exposed to RAF inhibitors, and it has been suggested that this may lead to the acceleration of the growth of such tumors (7,33). We found that induction of ERK phosphorylation in mutant RAS tumor cells induced only transient expression of some ERKdependent genes.…”

Section: Discussionsupporting

confidence: 62%

“…In contrast, although PLX4032 inhibited MEK and ERK phosphorylation in tumors with BRAF V600E , it rapidly induced MEK and ERK phosphorylation in all other tumor cells tested and in normal keratinocytes. Induction of ERK phosphorylation by other putative RAF inhibitors has been described recently (7,25,32) and suggests that paradoxical induction of ERK phosphorylation is common property of ATP-competitive RAF-kinase inhibitors in cells with BRAF WT , but not BRAF V600E (26,33). The mechanism of ERK induction in cells with BRAF WT has been attributed to negative feedback (23) or to selective inhibition of BRAF causing activation of CRAF (32).…”

Section: Discussionmentioning

confidence: 94%

“…T he prevalence of deregulation of ERK signaling in human tumors (1)(2)(3) suggests that drugs that inhibit the pathway might have significant therapeutic activity (4)(5)(6)(7). Selective, allosteric MAPK/ERK kinase (MEK) inhibitors (MEKi) have been useful for determining the utility and feasibility of therapeutic targeting of the ERK pathway.…”

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confidence: 99%

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The RAF inhibitor PLX4032 inhibits ERK signaling and tumor cell proliferation in a V600E BRAF-selective manner

Joseph

Pratilas

Poulikakos³

et al. 2010

Proc. Natl. Acad. Sci. U.S.A.

416

352

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Tumors with mutant BRAF and some with mutant RAS are dependent upon ERK signaling for proliferation, and their growth is suppressed by MAPK/ERK kinase (MEK) inhibitors. In contrast, tumor cells with human EGF receptor (HER) kinase activation proliferate in a MEK-independent manner. These findings have led to the development of RAF and MEK inhibitors as anticancer agents. Like MEK inhibitors, the RAF inhibitor PLX4032 inhibits the proliferation of BRAF V600E tumor cells but not that of HER kinase-dependent tumors. However, tumors with RAS mutation that are sensitive to MEK inhibition are insensitive to PLX4032. MEK inhibitors inhibit ERK phosphorylation in all normal and tumor cells, whereas PLX4032 inhibits ERK signaling only in tumor cells expressing BRAF V600E . In contrast, the drug activates MEK and ERK phosphorylation in cells with wildtype BRAF. In BRAF V600E tumor cells, MEK and RAF inhibitors affect the expression of a common set of genes. PLX4032 inhibits ERK signaling output in mutant BRAF cells, whereas it transiently activates the expression of these genes in tumor cells with wild-type RAF. Thus, PLX4032 inhibits ERK signaling output in a mutant BRAFselective manner. These data explain why the drug selectively inhibits the growth of mutant BRAF tumors and suggest that it will not cause toxicity resulting from the inhibition of ERK signaling in normal cells. This selectivity may lead to a broader therapeutic index and help explain the greater antitumor activity observed with this drug than with MEK inhibitors.

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Section: Discussionsupporting

confidence: 62%

Section: Discussionmentioning

confidence: 94%

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The RAF inhibitor PLX4032 inhibits ERK signaling and tumor cell proliferation in a V600E BRAF-selective manner

Joseph

Pratilas

Poulikakos³

et al. 2010

Proc. Natl. Acad. Sci. U.S.A.

416

352

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“…To identify potent inhibitors of dimeric BRAF, we compared eight structurally diverse RAF inhibitors: AZ-628 (AZ) (McDermott et al, 2007), TAK-632 (TAK) , LY3009120 (LY) (Peng et al, 2015), GDC-0879 (GDC) (Hoeflich et al, 2009), SB-590885 (SB) (King et al, 2006), PLX7904/Paradox Breaker (PB), which does not to induce paradoxical activation in wild-type BRAF cells , Vemurafenib (VEM) and Dabrafenib (DAB) (Rheault et al, 2013) (Figure S1A, Table S1). To compare potencies of inhibitors in cells endogenously expressing monomeric or dimeric BRAF V600E , we treated parental (PAR) SKMEL239 cells expressing full length BRAF V600E and the SKMEL239 derivative (clone C3) that is resistant to VEM due to enhanced dimerization of endogenous splice variants of BRAF V600E that lack the RAS-binding domain (Poulikakos et al, 2011).…”

Section: Structurally Diverse Raf Inhibitors Equi-potently Inhibit Momentioning

confidence: 99%

An Integrated Model of RAF Inhibitor Action Predicts Inhibitor Activity against Oncogenic BRAF Signaling

Karoulia¹,

Wu²,

Ahmed³

et al. 2016

Cancer Cell

127

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SUMMARYThe complex biochemical effects of RAF inhibitors account for both the effectiveness and mechanisms of resistance to these drugs, but a unified mechanistic model has been lacking. HereCorrespondence and requests for materials should be addressed to: Poulikos.poulikakos@mssm.edu or evripidis.gavathiotis@einstein.yu.edu. * These authors contributed equally to this work Accession numbers. Structural coordinates and parameters have been submitted to the Protein Database Bank under the following accession codes: 4RZV for BRAF R509H /VEM, 4RZW for BRAF R509H /AZ and 5ITA for BRAF WT /AZ-VEM. Other structural coordinates used in this study are the following: PDB ID: 4KSP for TAK bound to BRAF dimer, PDB ID: 3OG7 for VEM bound to BRAF V600E dimer, PDB ID: 4MNF for GDC bound to BRAF V600E dimer, PDB ID: 2FB8 for SB bound to BRAF dimer, PDB ID: 4XV2 for DAB bound to BRAF V600E dimer and PDB ID: 4XV1 for PB bound to BRAF V600E dimer and PDB 4MNE for the BRAF/MEK complex. AUTHOR CONTRIBUTIONSP.I.P., E.G., C.K., M.H., A.L., Z.K., Y.W. and T.A.A designed experiments. Z.K., T.A.A conducted biochemical and cellular studies. E.G., Y.W. performed structural determination and structural analysis. X.W. generated the CRAF-V5 CRISPR cell line. Q.X. synthesized the AZ-VEM compound. C.K., M.H., J.A.F., A.L., E.G., P.I.P. designed animal studies. Z.K., T.A.A and J.B. conducted animal experiments. C.Z. and G.B. provided reagents and analyzed data. P.I.P. and E.G. designed research, analyzed data and wrote the manuscript, which was edited by all authors.C.Z. and G.B. are employees of Plexxikon Inc. All other authors declare no competing financial interests.Publisher's Disclaimer: This is a PDF file of an unedited manuscript that has been accepted for publication. As a service to our customers we are providing this early version of the manuscript. The manuscript will undergo copyediting, typesetting, and review of the resulting proof before it is published in its final citable form. Please note that during the production process errors may be discovered which could affect the content, and all legal disclaimers that apply to the journal pertain. we show that RAF inhibitors exert their effects via two distinct allosteric mechanisms. Drug resistance due to dimerization is determined by the position of the αC-helix stabilized by inhibitor, whereas inhibitor-induced RAF priming and dimerization are the result of inhibitor-induced formation of the RAF/RAS-GTP complex. The biochemical effect of RAF inhibitor in cells is the combined outcome of the two mechanisms. Therapeutic strategies including αC-helix-IN inhibitors are more effective in multiple mutant BRAF-driven tumor models, including colorectal and thyroid BRAF V600E cancers, in which first generation RAF inhibitors have been ineffective. HHS Public Access

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“…Moreover, administration of GDC0879 significantly improved survival rates of mice harboring B-Raf mutant tumors in comparison with a control group of mice harboring Ras mutations (Hoeflich et al, 2009). GDC0879 inhibitory effect was strictly associated with V600E B-Raf mutations, which may limit its use for NSCLC, where V600E comprise only a minority of the B-Raf mutations.…”

Section: New Drugs In Clinical Developmentmentioning

confidence: 94%

BRAF mutations in non-small cell lung cancer: has finally Janus opened the door?

Caparica

Castro

Gil-Bazo

et al. 2016

Critical Reviews in Oncology/Hematology

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Antitumor Efficacy of the Novel RAF Inhibitor GDC-0879 Is Predicted by BRAFV600E Mutational Status and Sustained Extracellular Signal-Regulated Kinase/Mitogen-Activated Protein Kinase Pathway Suppression

Cited by 160 publications

References 25 publications

The RAF inhibitor PLX4032 inhibits ERK signaling and tumor cell proliferation in a V600E BRAF-selective manner

The RAF inhibitor PLX4032 inhibits ERK signaling and tumor cell proliferation in a V600E BRAF-selective manner

An Integrated Model of RAF Inhibitor Action Predicts Inhibitor Activity against Oncogenic BRAF Signaling

BRAF mutations in non-small cell lung cancer: has finally Janus opened the door?

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