CD200 is induced by ERK and is a potential therapeutic target in melanoma
Kimberly B. Petermann, … , Jonathan S. Serody, Norman E. Sharpless
Kimberly B. Petermann, … , Jonathan S. Serody, Norman E. Sharpless
Published November 15, 2007
Citation Information: J Clin Invest. 2007;117(12):3922-3929. https://doi.org/10.1172/JCI32163.
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Research Article Oncology

CD200 is induced by ERK and is a potential therapeutic target in melanoma

Abstract

Immune-mediated antitumor responses occur in patients with metastatic melanoma (MM), and therapies designed to augment such responses are clinically beneficial. Despite the immunogenicity of melanoma, immunomodulatory therapies fail in the majority of patients with MM. An inability of DCs to sufficiently activate effector cells may, in part, underlie this failure of the antitumor response seen in most patients. In this work, we show that mutation of N-RAS or B-RAF, signature genetic lesions present in most MMs, potently induced the expression of cell-surface CD200, a repressor of DC function. Employing 2 independent, genome-wide microarray analyses, we identified CD200 as a highly dynamic, downstream target of RAS/RAF/MEK/ERK activation in melanoma. CD200 protein was similarly overexpressed in human melanoma cell lines and primary tumors. CD200 mRNA expression correlated with progression and was higher in melanoma than in other solid tumors or acute leukemia. Melanoma cell lines expressing endogenous CD200 repressed primary T cell activation by DCs, while knockdown of CD200 by shRNA abrogated this immunosuppressive effect. These data indicate that in addition to its effects on growth, survival, and motility, ERK activation in MM attenuates a host antitumor immune response, implicating CD200 and its interaction with the CD200 receptor as a potential therapeutic target for MM.

Authors

Kimberly B. Petermann, Gabriela I. Rozenberg, Daniel Zedek, Pamela Groben, Karen McKinnon, Christin Buehler, William Y. Kim, Janiel M. Shields, Shannon Penland, James E. Bear, Nancy E. Thomas, Jonathan S. Serody, Norman E. Sharpless

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Figure 3

shRNA-mediated knockdown of CD200 expression.

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shRNA-mediated knockdown of CD200 expression. (A) WM2664 human melanoma ...
(A) WM2664 human melanoma cells were transduced with a GFP-expressing human CD200 shRNA construct and stained with an anti-human CD200 antibody (red). Untransduced WM2664 cells expressed CD200 (red). Transduced WM2664 cells were negative for CD200 expression. Nuclei of cells are stained with DAPI (blue). Original magnification, ×40. (B) CD200 expression at different passages in culture after transduction was analyzed by flow cytometry. Efficient knockdown of the CD200 protein was observed after 6 passages (>15 days) in culture. (C) WM2664 human melanoma cells were FACS sorted for GFP expression and then analyzed by immunofluorescence for CD200 expression. WM2664 cells transduced with a CD200 shRNA were negative for CD200 expression. WM2664 cells transduced with a nonspecific shRNA showed intense staining for CD200 (red). Original magnification, ×10.