Oncotarget

Research Papers:

TNF signaling mediates an enzalutamide-induced metastatic phenotype of prostate cancer and microenvironment cell co-cultures

Kai Sha, Shuyuan Yeh, Chawnshang Chang, Kent L. Nastiuk and John J. Krolewski _

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Oncotarget. 2015; 6:25726-25740. https://doi.org/10.18632/oncotarget.4535

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Abstract

Kai Sha1,5, Shuyuan Yeh1,2, Chawnshang Chang1,2,3,4, Kent L. Nastiuk1,5, John J. Krolewski1,4,5,6

1Department of Pathology and Laboratory Medicine, University of Rochester, School of Medicine and Dentistry; Rochester, NY 14642, USA

2Department of Urology, University of Rochester, School of Medicine and Dentistry; Rochester, NY 14642, USA

3Department of Radiation Oncology, University of Rochester, School of Medicine and Dentistry; Rochester, NY 14642, USA

4Wilmot Cancer Institute, University of Rochester, School of Medicine and Dentistry; Rochester, NY 14642, USA

5Department of Cancer Genetics, Roswell Park Cancer Institute, Buffalo, NY 14263

6Center for Personalized Medicine, Roswell Park Cancer Institute, Buffalo, NY 14263

Correspondence to:

John J. Krolewski, e-mail: [email protected]

Keywords: CCL2, enzalutamide, metastasis, microenvironment, TNF

Received: March 05, 2015     Accepted: July 17, 2015     Published: July 30, 2015

ABSTRACT

The dramatic responses tumors display to targeted therapies are limited by acquired or pre-existing mechanisms of therapy resistance. We recently discovered that androgen receptor blockade by the anti-androgen enzalutamide paradoxically enhanced metastasis and that these pro-metastatic effects were mediated by the chemoattractant CCL2. CCL2 is regulated by TNF, which is negatively regulated by androgen signaling. Thus, we asked if TNF mediates the pro-metastatic effects of enzalutamide. We found that androgen withdrawal or enzalutamide induced TNF mRNA and protein secretion in castration resistant prostate cancer (C4-2) cells, but not in macrophage-like (THP1) or myofibroblast-like (WPMY1) cells. Androgen deprivation therapy (ADT) induced autocrine CCL2 expression in C4-2 (as well as a murine CRPC cell line), while exogenous TNF induced CCL2 in THP1 and WPMY1. TNF was most potent in myofibroblast cultures, suggesting ADT induces CCL2 via paracrine interactions within the tumor microenvironment. A soluble TNF receptor (etanercept) blocked enzalutamide-induced CCL2 protein secretion and mRNA, implying dependence on secreted TNF. A small molecule inhibitor of CCR2 (the CCL2 receptor) significantly reduced TNF induced migration, while etanercept inhibited enzalutamide-induced migration and invasion of C4-2. Analysis of human prostate cancers suggests that a TNF-CCL2 paracrine loop is induced in response to ADT and might account for some forms of prostate cancer therapy resistance.


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