WNT5A enhances resistance of melanoma cells to targeted BRAF inhibitors
Jamie N. Anastas, … , Andy J. Chien, Randall T. Moon
Jamie N. Anastas, … , Andy J. Chien, Randall T. Moon
Published May 27, 2014
Citation Information: J Clin Invest. 2014;124(7):2877-2890. https://doi.org/10.1172/JCI70156.
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WNT5A enhances resistance of melanoma cells to targeted BRAF inhibitors

Abstract

About half of all melanomas harbor a mutation that results in a constitutively active BRAF kinase mutant (BRAFV600E/K) that can be selectively inhibited by targeted BRAF inhibitors (BRAFis). While patients treated with BRAFis initially exhibit measurable clinical improvement, the majority of patients eventually develop drug resistance and relapse. Here, we observed marked elevation of WNT5A in a subset of tumors from patients exhibiting disease progression on BRAFi therapy. WNT5A transcript and protein were also elevated in BRAFi-resistant melanoma cell lines generated by long-term in vitro treatment with BRAFi. RNAi-mediated reduction of endogenous WNT5A in melanoma decreased cell growth, increased apoptosis in response to BRAFi challenge, and decreased the activity of prosurvival AKT signaling. Conversely, overexpression of WNT5A promoted melanoma growth, tumorigenesis, and activation of AKT signaling. Similarly to WNT5A knockdown, knockdown of the WNT receptors FZD7 and RYK inhibited growth, sensitized melanoma cells to BRAFi, and reduced AKT activation. Together, these findings suggest that chronic BRAF inhibition elevates WNT5A expression, which promotes AKT signaling through FZD7 and RYK, leading to increased growth and therapeutic resistance. Furthermore, increased WNT5A expression in BRAFi-resistant melanomas correlates with a specific transcriptional signature, which identifies potential therapeutic targets to reduce clinical BRAFi resistance.

Authors

Jamie N. Anastas, Rima M. Kulikauskas, Tigist Tamir, Helen Rizos, Georgina V. Long, Erika M. von Euw, Pei-Tzu Yang, Hsiao-Wang Chen, Lauren Haydu, Rachel A. Toroni, Olivia M. Lucero, Andy J. Chien, Randall T. Moon

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Figure 7

WNT5A is upregulated as part of a gene signature associated with clinical phenotypes in melanoma.

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WNT5A is upregulated as part of a gene signature associated with clinica...
(A) The gene set upregulated in conjunction with WNT5A in BRAFi-resistant melanoma cells from Figure 1D was assessed in the previously published Mannheim data set, in which melanoma samples were clustered on the basis of either a highly metastatic phenotype (cohort C) or a less metastatic phenotype (cohorts A and B). The gene probes in the data set that were significant by ANOVA analysis (P < 0.01) are displayed in this heat map. Signal intensities are shown as log2-transformed data. (B) The same gene set from Figure 1D was assessed in the Broad Institute’s database of 88 melanoma samples (cell lines and short-term cultures). The heat map shows probes from the gene set that are significantly different (t test, P < 0.01) between samples with low and high expression of WNT5A.