AI Article Synopsis
- Stromal-epithelial cell interactions are crucial in cancer, making the tumor stroma a potential target for therapy.
- The study used a bioengineered microenvironment with human prostatic tissues to analyze how cancer-associated fibroblasts (CAFs) influence non-tumorigenic BPH-1 epithelial cells compared to non-malignant prostatic fibroblasts (NPFs).
- Co-culturing BPH-1 cells with CAFs led to a more invasive and mobile cell phenotype, indicating that tumor stroma significantly affects prostate cancer progression, regardless of the aggressiveness of the tumor type.
Article Abstract
Stromal-epithelial cell interactions play an important role in cancer and the tumor stroma is regarded as a therapeutic target. In vivo xenografting is commonly used to study cellular interactions not mimicked or quantified in conventional 2D culture systems. To interrogate the effects of tumor stroma (cancer-associated fibroblasts or CAFs) on epithelia, we created a bioengineered microenvironment using human prostatic tissues. Patient-matched CAFs and non-malignant prostatic fibroblasts (NPFs) from men with moderate (Gleason 7) and aggressive (Gleason 8-9 or castrate-resistant) prostate cancer were cultured with non-tumorigenic BPH-1 epithelial cells. Changes in the morphology, motility and phenotype of BPH-1 cells in response to CAFs and NPFs were analyzed using immunofluorescence and quantitative cell morphometric analyses. The matrix protein gene expression of CAFs, with proven tumorigenicity in vivo, had a significantly different gene expression profile of matrix proteins compared to patient matched NPFs. In co-culture with CAFs (but not NPFs), BPH-1 cells had a more invasive, elongated phenotype with increased motility and a more directed pattern of cell migration. CAFs from more aggressive tumors (Gleason 8-9 or CRPC) were not quantitatively different to moderate grade CAFs. Overall, our bioengineered microenvironment provides a novel 3D in vitro platform to systematically investigate the effects of tumor stroma on prostate cancer progression.
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| http://dx.doi.org/10.1016/j.biomaterials.2013.03.005 | DOI Listing |
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