MERTK receptor tyrosine kinase is a therapeutic target in melanoma
Jennifer Schlegel, … , Janiel M. Shields, Douglas K. Graham
Jennifer Schlegel, … , Janiel M. Shields, Douglas K. Graham
Published April 15, 2013
Citation Information: J Clin Invest. 2013;123(5):2257-2267. https://doi.org/10.1172/JCI67816.
View: Text | PDF
Research Article Oncology

MERTK receptor tyrosine kinase is a therapeutic target in melanoma

Abstract

Metastatic melanoma is one of the most aggressive forms of cutaneous cancers. Although recent therapeutic advances have prolonged patient survival, the prognosis remains dismal. C-MER proto-oncogene tyrosine kinase (MERTK) is a receptor tyrosine kinase with oncogenic properties that is often overexpressed or activated in various malignancies. Using both protein immunohistochemistry and microarray analyses, we demonstrate that MERTK expression correlates with disease progression. MERTK expression was highest in metastatic melanomas, followed by primary melanomas, while the lowest expression was observed in nevi. Additionally, over half of melanoma cell lines overexpressed MERTK compared with normal human melanocytes; however, overexpression did not correlate with mutations in BRAF or RAS. Stimulation of melanoma cells with the MERTK ligand GAS6 resulted in the activation of several downstream signaling pathways including MAPK/ERK, PI3K/AKT, and JAK/STAT. MERTK inhibition via shRNA reduced MERTK-mediated downstream signaling, reduced colony formation by up to 59%, and diminished tumor volume by 60% in a human melanoma murine xenograft model. Treatment of melanoma cells with UNC1062, a novel MERTK-selective small-molecule tyrosine kinase inhibitor, reduced activation of MERTK-mediated downstream signaling, induced apoptosis in culture, reduced colony formation in soft agar, and inhibited invasion of melanoma cells. This work establishes MERTK as a therapeutic target in melanoma and provides a rationale for the continued development of MERTK-targeted therapies.

Authors

Jennifer Schlegel, Maria J. Sambade, Susan Sather, Stergios J. Moschos, Aik-Choon Tan, Amanda Winges, Deborah DeRyckere, Craig C. Carson, Dimitri G. Trembath, John J. Tentler, S. Gail Eckhardt, Pei-Fen Kuan, Ronald L. Hamilton, Lyn M. Duncan, C. Ryan Miller, Nana Nikolaishvili-Feinberg, Bentley R. Midkiff, Jing Liu, Weihe Zhang, Chao Yang, Xiaodong Wang, Stephen V. Frye, H. Shelton Earp, Janiel M. Shields, Douglas K. Graham

×

Figure 1

MERTK expression in nevus and melanoma tissues.

Options: View larger image (or click on image) Download as PowerPoint
MERTK expression in nevus and melanoma tissues. (A) Box plots of MERTK e...
(A) Box plots of MERTK expression in nevus, primary, and metastatic melanoma human samples. AQUA score of MERTK expression for each of the TMA cores representing nevi, primary, and metastatic melanoma were calculated in S100-positive cells and were normalized using logarithmic transformation. (B) Representative tissue cores from the nevus-to-melanoma TMA. Original magnification, ×20. Core H&E-stained images (top). Merged images (RGB) showing S100 staining pseudocolored with green and MERTK protein pseudocolored with red (bottom). (C) MERTK expression in a representative tissue section from a patient who underwent craniotomy for melanoma brain metastases. Tissues were stained for MERTK using alkaline phosphatase (red) detection and counterstained with hematoxylin. Original magnification, ×40. (D) Representative tissue core from the UNC metastatic melanoma TMA stained with H&E (left) and merged image showing staining with CD68 (pseudocolored with green), MERTK protein (pseudocolored with red), and Hoechst (blue, right). (E) Gene expression analysis of MERTK transcript in patient tissue samples from the GSE7553 microarray dataset (*P < 0.05, Tukey’s multiple comparison test).