Oncogenic BRAF is Required for Tumor Growth and Maintenance in Melanoma Models

Overview

Journal Cancer Res

Specialty Oncology

Date 2006 Jan 21

PMID 16424035

Citations 94

Authors

Klaus P Hoeflich

Daniel C Gray

Michael T Eby

Janet Y Tien

Leo Wong

Janeko Bower

Alvin Gogineni

Jiping Zha

Mary J Cole

Howard M Stern

Lesley J Murray

David P Davis

Somasekar Seshagiri

Affiliations

Soon will be listed here.

Abstract

The usual paradigm for developing kinase inhibitors in oncology is to use a high-affinity proof-of-concept inhibitor with acceptable metabolic properties for key target validation experiments. This approach requires substantial medicinal chemistry and can be confounded by drug toxicity and off-target activities of the test molecule. As a better alternative, we have developed inducible short-hairpin RNA xenograft models to examine the in vivo efficacy of inhibiting oncogenic BRAF. Our results show that tumor regression resulting from BRAF suppression is inducible, reversible, and tightly regulated in these models. Analysis of regressing tumors showed the primary mechanism of action for BRAF to be increased tumor cell proliferation and survival. In a metastatic melanoma model, conditional BRAF suppression slowed systemic tumor growth as determined by in vivo bioluminescence imaging. Taken together, gain-of-function BRAF signaling is strongly associated with in vivo tumorigenicity, confirming BRAF as an important target for small-molecule and RNA interference-based therapeutics.

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