TY - JOUR
T1 - PDGFRB promotes liver metastasis formation of mesenchymal-like colorectal tumor cells
AU - Steller, Ernst J.A.
AU - Raats, Danielle A.
AU - Koster, Jan
AU - Rutten, Bert
AU - Govaert, Klaas M.
AU - Emmink, Benjamin L.
AU - Snoeren, Nikol
AU - van Hooff, Sander R.
AU - Holstege, Frank C.P.
AU - Maas, Coen
AU - Rinkes, Inne H.M.Borel
AU - Kranenburg, Onno
N1 - Funding Information:
Abbreviations: CRC, colorectal cancer; CRP, collagen-related peptide; DAPI, 4′,6-diamidino-2-phenylindole; DFS, disease-free survival; ECM, extracellular matrix; EGFR, epithelial growth factor receptor; EMT, epithelial-to-mesenchymal transition; FCS, fetal calf serum; GFP, green fluorescent protein; HRA, hepatic replacement area; OS, overall survival; PDGF, platelet-derived growth factor; PDGFR, platelet-derived growth factor receptor; TGFBR, transforming growth factor beta receptor; TRAP, thrombin receptor– activating peptide Address all correspondence to: Onno Kranenburg, PhD, Department of Surgery, University Medical Center Utrecht, Heidelberglaan 100, 3584CX Utrecht, The Netherlands. E-mail: [email protected] 1This work was supported by grants from the Dutch Cancer Society (E.J.A.S.; 2009-4379/D.A.R.; 2009-4417/B.L.E.; 2009-4367/K.M.G.; 2010-4608/N.S.; 2007-3923), the PON Foundation, and the Netherlands Organization for Scientific Research (C.M.; 016-126-159). Conflict of interest: None. 2This article refers to supplementary materials, which are designated by Table W1 and Figures W1 to W7 and are available online at www.neoplasia.com. Received 15 October 2012; Revised 13 December 2012; Accepted 14 December 2012 Copyright © 2013 Neoplasia Press, Inc. All rights reserved 1522-8002/13/$25.00 DOI 10.1593/neo.121726
PY - 2013/2
Y1 - 2013/2
N2 - In epithelial tumors, the platelet-derived growth factor receptor B (PDGFRB) is mainly expressed by stromal cells of mesenchymal origin. Tumor cells may also acquire PDGFRB expression following epithelial-to-mesenchymal transition (EMT), which occurs during metastasis formation. Little is known about PDGFRB signaling in colorectal tumor cells. We studied the relationship between PDGFRB expression, EMT, and metastasis in human colorectal cancer (CRC) cohorts by analysis of gene expression profiles. PDGFRB expression in primary CRC was correlated with short disease-free and overall survival. PDGFRB was co-expressed with genes involved in platelet activation, transforming growth factor beta (TGFB) signaling, and EMT in three CRC cohorts. PDGFRB was expressed in mesenchymal-like tumor cell lines in vitro and stimulated invasion and liver metastasis formation in mice. Platelets, a major source of PDGF, preferentially bound to tumor cells in a non-activated state. Platelet activation caused robust PDGFRB tyrosine phosphorylation on tumor cells in vitro and in liver sinusoids in vivo. Platelets also release TGFB, which is a potent inducer of EMT. Inhibition of TGFB signaling in tumor cells caused partial reversion of the mesenchymal phenotype and strongly reduced PDGFRB expression and PDGF-stimulated tumor cell invasion. These results suggest that PDGFRB may contribute to the aggressive phenotype of colorectal tumors with mesenchymal properties, most likely downstream of platelet activation and TGFB signaling.
AB - In epithelial tumors, the platelet-derived growth factor receptor B (PDGFRB) is mainly expressed by stromal cells of mesenchymal origin. Tumor cells may also acquire PDGFRB expression following epithelial-to-mesenchymal transition (EMT), which occurs during metastasis formation. Little is known about PDGFRB signaling in colorectal tumor cells. We studied the relationship between PDGFRB expression, EMT, and metastasis in human colorectal cancer (CRC) cohorts by analysis of gene expression profiles. PDGFRB expression in primary CRC was correlated with short disease-free and overall survival. PDGFRB was co-expressed with genes involved in platelet activation, transforming growth factor beta (TGFB) signaling, and EMT in three CRC cohorts. PDGFRB was expressed in mesenchymal-like tumor cell lines in vitro and stimulated invasion and liver metastasis formation in mice. Platelets, a major source of PDGF, preferentially bound to tumor cells in a non-activated state. Platelet activation caused robust PDGFRB tyrosine phosphorylation on tumor cells in vitro and in liver sinusoids in vivo. Platelets also release TGFB, which is a potent inducer of EMT. Inhibition of TGFB signaling in tumor cells caused partial reversion of the mesenchymal phenotype and strongly reduced PDGFRB expression and PDGF-stimulated tumor cell invasion. These results suggest that PDGFRB may contribute to the aggressive phenotype of colorectal tumors with mesenchymal properties, most likely downstream of platelet activation and TGFB signaling.
UR - http://www.scopus.com/inward/record.url?scp=84873505703&partnerID=8YFLogxK
U2 - 10.1593/neo.121726
DO - 10.1593/neo.121726
M3 - Article
AN - SCOPUS:84873505703
SN - 1522-8002
VL - 15
SP - 204
EP - 217
JO - Neoplasia (United States)
JF - Neoplasia (United States)
IS - 2
ER -