Paracrine communication between malignant and non-malignant prostate epithelial cells in culture alters growth rate, matrix protease secretion and in vitro invasion

被引:0
作者
Andrea H. Greiff
William M. Fischer
Inder Sehgal
机构
[1] North Dakota State University,Department of Pharmaceutical Sciences, Center for Protease Research
[2] North Dakota State University,Center for Protease Research
来源
Clinical & Experimental Metastasis | 2002年 / 19卷
关键词
co-culture; invasion; matrix metalloproteinase (MMP); prostate cancer; TGFβ1;
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学科分类号
摘要
Epithelial cancer cell invasion is facilitated by stromal cells, immune cells, endothelial cells and other epithelial cells. We have used two human papilloma immortalized prostate cell lines, CA-HPV-10 from a carcinoma and PZ-HPV-7 cells from normal prostatic epithelium to study cell–cell influences on growth, gelatinase secretion, invasion and responses to TGFβ1. We found that co-culture with CA-10 carcinoma cells stimulates proliferation of the PZ-7 epithelial line. TGFβ1 inhibited growth of both lines, but while inhibitory effects on the CA-10 cells diminished after removal of the peptide, inhibition of PZ-7 was lasting. Interestingly, the TGFβ-induced growth inhibition in PZ-7 cells could be partially reversed by co-culture with CA-10 cells. Co-culture with CA cells in a 3-chamber invasion assay also promoted invasion of PZ cells. CA-10 invasion was enhanced by co-culture with TGFβ1-treated-PZ-7 cultures and this enhancement was associated with TGFβ1-induced secretion of matrix metalloproteinase-9. Our observations suggest that interaction between prostate cancer cells and prostate epithelial cells may promote proliferation of the epithelial cell population and produce a paracrine source of MMP-9 which may facilitate early cancer cell invasion.
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页码:727 / 733
页数:6
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