Enhanced Hepatocyte Growth Factor Signaling by Type II Transforming Growth Factor-{beta} Receptor Knockout Fibroblasts Promotes Mammary Tumorigenesis

doi:10.1158/0008-5472.CAN-06-3381

Cell Death Mechanisms and Cancer Therapy

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Published online first on May 10, 2007
[Cancer Research, 10.1158/0008-5472.CAN-06-3381]

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Experimental Therapeutics, Molecular Targets, and Chemical Biology

Enhanced Hepatocyte Growth Factor Signaling by Type II Transforming Growth Factor- ${beta}$ Receptor Knockout Fibroblasts Promotes Mammary Tumorigenesis

Nikki Cheng ¹, Anna Chytil , Yu Shyr , Alison Joly , Harold L. Moses ^*

¹ Departments of ¹Cancer Biology and ²Pathology, ³Biostatistics Core Facility, and ⁴Vanderbilt-Ingram Cancer Center, Vanderbilt University School of Medicine, Nashville, Tennessee; and ⁵Exelixis, Inc., South San Francisco, California

^* To whom correspondence should be addressed. E-mail: Hal.Moses{at}vanderbilt.edu.

Abstract

Transforming growth factor- ${beta}$ (TGF- ${beta}$ ) plays complex dual rolesas an inhibitor and promoter of tumor progression. Althoughthe influence of the stromal microenvironment on tumor progressionis well recognized, little is known about the functions of TGF- ${beta}$ signaling in the stroma during tumor progression. Using cre-loxtechnology, expression of the type II TGF- ${beta}$ receptor was selectivelyknocked out in fibroblasts (Tgfbr2^FspKO). In a co-xenograftmodel, we show that Tgfbr2^FspKO fibroblasts enhance mammarycarcinoma growth and metastasis in mice while increasing hepatocytegrowth factor (HGF) expression and c-Met signaling downstreampathways including signal transducers and activators of transcription3 (Stat3) and p42/44 mitogen-activated protein kinase (MAPK).Treatment of tumor-bearing mice with a pharmacologic inhibitor(EXEL-7592) of c-Met blocks tumor progression and reduces levelsof phospho-Stat3 and phospho-p42/44 MAPK. Similarly, small interferingRNA knockdown of c-Met expression in mammary tumor cells reducesmetastasis and c-Met signaling caused by Tgfbr2^FspKO fibroblasts.The results show that TGF- ${beta}$ signaling in fibroblasts suppressestumor metastasis by antagonizing HGF/c-Met signaling withintumor epithelial cells. Furthermore, this co-xenograft modelrepresents a unique context to study stromal TGF- ${beta}$ and HGF signalingin mammary tumorigenesis. [Cancer Res 2007;67(10):4869-77]

Key Words: c-Met, HGF, mammary tumor progression, stromal-epithelial interactions, type II TGF- ${beta}$ receptor

This article has been cited by other articles:

N. Cheng, A. Chytil, Y. Shyr, A. Joly, and H. L. Moses
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Mol. Cancer Res., October 1, 2008; 6(10): 1521 - 1533.
[Abstract] [Full Text] [PDF]