Tumor endothelin-1 enhances metastatic colonization of the lung in mouse xenograft models of bladder cancer
Neveen Said, … , Marta Sanchez-Carbayo, Dan Theodorescu
Neveen Said, … , Marta Sanchez-Carbayo, Dan Theodorescu
Published December 22, 2010
Citation Information: J Clin Invest. 2011;121(1):132-147. https://doi.org/10.1172/JCI42912.
View: Text | PDF
Research Article Oncology

Tumor endothelin-1 enhances metastatic colonization of the lung in mouse xenograft models of bladder cancer

Abstract

Many patients with advanced bladder cancer develop lethal metastases to the lung. The vasoconstricting protein endothelin-1 (ET-1) has been implicated in this process, although the mechanism(s) by which it promotes metastasis remains unclear. Here, we have evaluated whether tumor ET-1 expression can serve as a biomarker for lung metastasis and whether it is required for metastatic disease. Evaluation of ET-1 mRNA and protein expression in four patient cohorts revealed that levels of ET-1 are higher in patients with muscle-invasive bladder cancers, which are associated with higher incidence of metastasis, and that high ET-1 levels are associated with decreased disease-specific survival. Consistent with its proinflammatory activity, we found that tumor-derived ET-1 acts through endothelin-1 receptor A (ETAR) to enhance migration and invasion of both tumor cells and macrophages and induces expression of inflammatory cytokines and proteases. Using human and mouse cancer cells depleted of ET-1 and pharmacologic blockade of ET receptors in lung metastasis models, we found that tumor ET-1 expression and ETAR activity are necessary for metastatic lung colonization and that this process is preceded by and dependent on macrophage infiltration of the lung. In contrast, tumor ET-1 expression and ETAR activity appeared less important in established primary or metastatic tumor growth. These findings strongly suggest that ETAR inhibitors might be more effective as adjuvant therapeutic agents than as initial treatment for advanced primary or metastatic disease.

Authors

Neveen Said, Steven Smith, Marta Sanchez-Carbayo, Dan Theodorescu

×

Figure 1

The association between the expression ET family genes, muscle invasion, and DSS in human bladder cancer.

Options: View larger image (or click on image) Download as PowerPoint
The association between the expression ET family genes, muscle invasion,...
(AF) Datasets were used from Sanchez-Carbayo et al. (S-C et al.) (n = 26 and 65 for NMI and MI disease, respectively), GSE13507 (n = 103 and 62 for NMI and MI disease, respectively), and UVA-Den (n = 36 and 24, for NMI and MI, respectively). Data for the expression of ET1 (A), ECE1 (B), ETAR (C) were plotted using probesets identified in Methods. Dot plots represent standardized (z-scored) logged (base 2) expression of probes comparing NMI and MI tumors, and differences in distributions were tested by the Mann-Whitney U test. Kaplan-Meier curves show the association between expression of ET1 (D), ECE1 (E), and ETAR (F) expression and DSS of patients (log-rank). (G) Typical immunohistochemical staining of ET-1 in NMI and MI bladder cancer TMAs (total magnification, ×200). Kaplan-Meier curves reveal association of ET-1 protein expression as assessed by immunohistochemistry in 92 NMI and 102 MI tumor and DSS. Bladder cancer TMAs and IHC protocols and scoring are described in Methods.