10 research outputs found
QUANTITATIVE ANALYSIS OF TUMOUR CELL BURDEN IN METASTATIC PROSTATE CANCER USING LYMPH NODE DISINTEGRATES
No full textACTIVATION COMBINED BIOMARKERS PI3K AND P-AKT IS ASSOCIATED WITH REDUCED SURVIVAL IN RENAL CELL CARCINOMA
No full textLocal diversivity of mTOR pathway markers’ of tissue expression in prostate cancer and implications of a prognostic role
No full text442 Increased rates of false positive urine based bladder cancer markers due to impaired renal function
No full text841 Farnesyl pyrophosphate synthase – the target enzyme of zoledronic acid is increasingly expressed in prostate cancer tissue
No full text114 Systemic alterations of Wnt Inhibitors in patients with prostate cancer and bone metastases
No full text429 PCR-based detection of circulating tumor cells in prostate cancer – preliminary experience
No full textInsulin receptor isoforms A and B as well as insulin receptor substrates-1 and -2 are differentially expressed in prostate cancer.
Get PDFAims/Hypothesis: In different cancers types, insulin receptor isoform composition or insulin receptor substrate (IRS) isoforms are different to healthy tissue. This may be a molecular link to increased cancer risk in diabetes and obesity. Since this is yet unclear for prostate cancer, we investigated IR isoform composition and IRS balance in prostate cancer compared to benign and tumor adjacent benign prostate tissue and brought this into relation to cell proliferation. Methods: We studied 23 benign prostate samples from radical cystectomy or benign prostatic hyperplasia surgery, 30 samples from benign tissue directly adjacent to prostate cancer foci and 35 cancer samples from different patients. RNA expression levels for insulin receptor isoforms A and B, IRS-1, IRS-2, and IGF-1 receptor were assessed by quantitative real-time RT-PCR. In addition, RNA-and protein expression of the cell cycle regulator p27(Kip1) was quantified by real-time RT-PCR and immunohistochemistry. Results: Insulin receptor isoform A to B ratio was significantly higher in cancer as well as in tumor adjacent benign prostate tissue compared to purely benign prostates (p<0.05). IRS-1 to IRS-2 ratios were lower in malignant than in benign prostatic tissue (p<0.05). These altered ratios both in cancer and adjacent tissue were significantly associated with reduced p27(Kip1) content (p<0.02). Interestingly, IGF-1 receptor levels were significantly lower in patients with type 2 diabetes (p = 0.0019). Conclusions/Interpretation: We found significant differences in the insulin signaling cascade between benign prostate tissue and prostate cancer. Histological benign tissue adjacent to cancer showed expression patterns similar to the malignancies. Our findings suggest a role of the insulin signaling pathway in prostate cancer and surrounding tissue and can hence be relevant for both novel diagnostic and therapeutic approaches in this malignancy
