AI Article Synopsis
- Prostate cancer varies greatly in severity, ranging from slow-growing forms to aggressive types, but existing research cell lines mostly come from advanced cases, highlighting the need for new lines from early-stage localized disease.
- Researchers established four new cell lines from patients with localized prostate cancer, two from benign tissue and two from tumor tissue, using techniques like HPV16 immortalization and RNA sequencing to analyze their characteristics.
- The new cell lines retained an epithelial structure and showed a slower growth rate, differing significantly in gene expression from common metastatic prostate cancer cell lines, which may be important for further understanding of the disease's early stages.
Article Abstract
Background: Prostate cancer is a broad-spectrum disease, spanning from indolent to a highly aggressive lethal malignancy. Prostate cancer cell lines are essential tools to understanding the basic features of this malignancy, as well as in identifying novel therapeutic strategies. However, most cell lines routinely used in prostate cancer research are derived from metastatic disease and may not fully elucidate the molecular events underlying the early stages of cancer development and progression. Thus, there is a need for new cell lines derived from localised disease to better span the disease spectrum.
Methods: Prostatic tissue from the primary site, and adjacent non-cancerous tissue was obtained from four patients with localised disease undergoing radical prostatectomy. Epithelial cell outgrowths were immortalised with human papillomavirus type 16 (HPV16) E6 and E7 to establish monoclonal cell lines. Chromosomal ploidy was imaged and STR profiles were determined. Cell morphology, colony formation and cell proliferation characteristics were assessed. Androgen receptor (AR) expression and AR-responsiveness to androgen treatment were analysed by immunofluorescence and RT-qPCR, respectively. RNA-seq analysis was performed to identify prostate lineage markers and expression of prostate cancer tumorigenesis-related genes.
Results: Two benign cell lines derived from non-cancer cells (AQ0420 and AQ0396) and two tumour tissue derived cancer cell lines (AQ0411 and AQ0415) were immortalised from four patients with localised prostatic adenocarcinoma. The cell lines presented an epithelial morphology and a slow to moderate proliferative rate. None of the cell lines formed anchorage independent colonies or displayed AR-responsiveness. Comparative RNA-seq expression analysis confirmed the prostatic lineage of the four cell lines, with a distinct gene expression profile from that of the metastatic prostate cancer cell lines, PC-3 and LNCaP.
Conclusions: Comprehensive characterization of these cell lines may provide new in vitro tools that could bridge the current knowledge gap between benign, early-stage and metastatic disease.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10449630 | PMC |
| http://dx.doi.org/10.1038/s41391-023-00679-x | DOI Listing |
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