Loss of type III transforming growth factor {beta} receptor expression increases motility and invasiveness associated with epithelial to mesenchymal transition during pancreatic cancer progression

doi:10.1093/carcin/bgm249

Carcinogenesis Advance Access originally published online on November 13, 2007
Carcinogenesis 2008 29(2):252-262; doi:10.1093/carcin/bgm249

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Loss of type III transforming growth factor β receptor expression increases motility and invasiveness associated with epithelial to mesenchymal transition during pancreatic cancer progression

Kelly J. Gordon¹, Mei Dong², Elizabeth M. Chislock¹, Timothy A. Fields³ and Gerard C. Blobe¹^,2^,*

¹ Department of Pharmacology and Cancer Biology
² Department of Medicine
³ Department of Pathology, Duke University Medical Center, Durham, NC 27710, USA

^* To whom correspondence should be addressed. Tel: +1 919 668 1352; Fax: +1 919 668 2458; Email: blobe001{at}mc.duke.edu

Epithelial to mesenchymal transitions (EMTs) contribute to increasesin cellular motility and invasiveness during embryonic developmentand tumorigenesis. The transforming growth factor β (TGF-β)signaling pathway is a key regulator of EMT. The TGF-βsuperfamily coreceptor, the type III TGF-β receptor (TβRIIIor betaglycan), is required for EMT during embryonic heart developmentand palate fusion. Here, we establish that in a pancreatic cancermodel of EMT, TβRIII expression is specifically lost duringEMT at the mRNA and protein levels, whereas levels of the TGF-βtype I and type II receptors are maintained at the mRNA level.Loss of TβRIII expression at the protein level precedesthe loss of E-cadherin and cytoskeletal reorganization duringearly stages of EMT. However, maintaining TβRIII expressiondoes not block these aspects of EMT, but instead suppressesthe increased motility and invasiveness associated with EMT.Reciprocally, shRNA-mediated knockdown of endogenous TβRIIIincreases cellular motility without affecting Snail or E-cadherinlevels. The ability of TβRIII to suppress motility andinvasiveness does not depend on its cytoplasmic domain or itscoreceptor function. Instead, this suppression of invasion ispartially mediated by ectodomain shedding of TβRIII, generatingsoluble TβRIII (sTβRIII). In human pancreatic cancerspecimens, TβRIII expression decreases at both the mRNAand protein levels, with the degree of loss correlating withworsening tumor grade. Taken together, these studies supporta role for loss of TβRIII expression during the EMT ofpancreatic cancer progression, with a specific role for sTβRIIIin suppressing EMT-associated increases in motility and invasion.

Abbreviations: CM, conditioned media; EMT, epithelial to mesenchymal transition; NTC, non-targeting control; sTβRIII, soluble TβRIII; TGF-β, transforming growth factor β

Received July 30, 2007; revised October 30, 2007; accepted November 3, 2007.

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