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

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

Cancer Research	Clinical Cancer Research
Cancer Epidemiology Biomarkers & Prevention	Molecular Cancer Therapeutics
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Published online first on March 10, 2009
[Cancer Research, 10.1158/0008-5472.CAN-08-3563]

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Experimental Therapeutics, Molecular Targets and Chemical Biology

Antitumor Efficacy of the Novel RAF Inhibitor GDC-0879 Is Predicted by BRAF^V600E Mutational Status and Sustained Extracellular Signal-Regulated Kinase/Mitogen-Activated Protein Kinase Pathway Suppression

Klaus P. Hoeflich ¹, Sylvia Herter ¹, Janet Tien ¹, Leo Wong ¹, Leanne Berry ¹, Jocelyn Chan ¹, Carol O'Brien ², Zora Modrusan ³, Somasekar Seshagiri ³, Mark Lackner ², Howard Stern ⁴, Edna Choo ⁵, Lesley Murray ^{1, 5}, Lori S. Friedman ¹, Marcia Belvin ¹^*

Departments of ¹Cancer Signaling and Translational Oncology, ²Molecular Diagnostics, ³Molecular Biology, ⁴Pathology, and ⁵Drug Metabolism and Pharmacokinetics, Genentech, Inc., South San Francisco, California

^* To whom correspondence should be addressed. E-mail: mbelvin{at}gene.com.

Abstract

Oncogenic activation of the BRAF serine/threonine kinase hasbeen associated with initiation and maintenance of melanomatumors. As such, development of pharmacologic agents to targetRAF proteins or their effector kinases is an area of intenseinvestigation. Here we report the biological properties of GDC-0879,a highly selective, potent, and orally bioavailable RAF small-moleculeinhibitor. We used extracellular signal-regulated kinase (ERK)-1/2and mitogen-activated protein kinase/ERK kinase (MEK)-1/2 phosphorylationas biomarkers to explore the relationship between tumor outcomeand pharmacodynamic inhibition of the RAF-MEK-ERK pathway. InGDC-0879–treated mice, both cell line– and patient-derivedBRAF^V600E tumors exhibited stronger and more sustained pharmacodynamicinhibition (>90% for 8 hours) and improved survival comparedwith mutant KRAS–expressing tumors. Despite the involvementof activated RAF signaling in RAS-induced tumorigenesis, decreasedtime to progression was observed for some KRAS-mutant tumorsfollowing GDC-0879 administration. Moreover, striking differenceswere noted for RAF and MEK inhibition across a panel of 130tumor cell lines. Whereas GDC-0879–mediated efficacy wasassociated strictly with BRAF^V600E status, MEK inhibition alsoattenuated proliferation and tumor growth of cell lines expressingwild-type BRAF (81% KRAS mutant, 38% KRAS wild type). The responsivenessof BRAF^V600E melanoma cells to GDC-0879 could be dramaticallyaltered by pharmacologic and genetic modulation of phosphatidylinositol3-kinase pathway activity. These data suggest that GDC-0879–inducedsignaling changes are dependent on the point of oncogenic activationwithin the RAS network. Taken together, these studies increaseour understanding of the molecular determinants for antitumorefficacy resulting from RAF pathway inhibition and have implicationsfor therapeutic intervention in the clinic. [Cancer Res 2009;69(7):OF1–10]

Key Words: BRAF, inhibitor, KRAS