Overexpression of PDGF-BB decreases colorectal and pancreatic cancer growth by increasing tumor pericyte content
Marya F. McCarty, … , Corazon Bucana, Lee M. Ellis
Marya F. McCarty, … , Corazon Bucana, Lee M. Ellis
Published August 1, 2007
Citation Information: J Clin Invest. 2007;117(8):2114-2122. https://doi.org/10.1172/JCI31334.
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Research Article Oncology

Overexpression of PDGF-BB decreases colorectal and pancreatic cancer growth by increasing tumor pericyte content

Abstract

We hypothesized that overexpression of PDGF-BB in colorectal cancer (CRC) and pancreatic cancer cells would result in increased pericyte coverage of ECs in vivo, rendering the tumor vasculature more resistant to antiangiogenic therapy. We stably transfected the cDNA for the PDGF-B into HT-29 human CRC and FG human pancreatic cancer cells. Surprisingly, when HT-29 or FG parental and transfected cells were injected into mice (subcutaneously and orthotopically), we observed marked inhibition of tumor growth in the PDGF-BB–overexpressing clones. In the PDGF-BB–overexpressing tumors, we observed an increase in pericyte coverage of ECs. Treatment of PDGF-BB–overexpressing tumors with imatinib mesylate (PDGFR inhibitor) resulted in increased growth and decreased total pericyte content compared with those in untreated PDGF-BB–overexpressing tumors. In vitro studies demonstrated the ability of VSMCs to inhibit EC proliferation by approximately 50%. These data show that increasing the pericyte content of the tumor microenvironment inhibits the growth of angiogenesis-dependent tumors. Single-agent therapy targeting PDGF receptor must be used with caution in tumors when PDGFR is not the target on the tumor cell itself.

Authors

Marya F. McCarty, Ray J. Somcio, Oliver Stoeltzing, Jane Wey, Fan Fan, Wenbiao Liu, Corazon Bucana, Lee M. Ellis

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Figure 1

Effect of PDGF-BB overexpression on growth of subcutaneous tumors.

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Effect of PDGF-BB overexpression on growth of subcutaneous tumors. Human...
Human colon cancer cell lines HT-29 (parental), HT-29 Neo pool, HT-29 S2 (PDGF-BB–overexpressing), and HT-29 S4 (PDGF-BB–overexpressing) (1 × 106) were injected subcutaneously into nude mice. (A) Tumor growth was measured 3 times weekly (Monday, Wednesday, and Friday) until tumors became necrotic or larger than 1 cm3. (B) Photomicrographs of representative tumors from each group. HT-29 S2 and HT-29 S4 cells demonstrated decreased tumor growth and a significant reduction in end-stage tumor mass in vivo. *P < 0.05. Original magnification, ×1.