The steroid receptor coactivator-3 is required for developing neuroendocrine tumor in the mouse prostate. Academic Article

abstract

• Neuroendocrine tumor cells (NETCs) are commonly observed in prostate cancer. Their presence is associated with castration resistance, metastasis and poor prognosis. Cellular and molecular mechanisms for NETC initiation and growth are unknown. TRAMP mice develop heterogeneous adenocarcinomas induced by expression of the SV40-T/t oncogene in prostate epithelial cells. Here, we demonstrate prostate tumors in TRAMP mice with a mixed genetic background are characterized mostly by atypical hyperplasia (AH) containing steroid receptor coactiator-3-positive, androgen receptor-positive and synaptophysin-negative (SRC-3+/AR+/Syp-) cells. Few SRC-3+/AR-/Syp+ NETCs are present in their prostates. We generated TRAMP mice in which SRC-3 was specifically ablated in AR+/Syp- prostatic epithelial cells (termed PE3KOT mice). In these animals, we observed a substantial reduction in SRC-3-/AR+/Syp- AH tumor growth. There was a corresponding increase in SRC-3-/AR+/Syp- phyllodes lesions, suggesting SRC-3 knockout can convert aggressive AH tumors with mostly epithelial tumor cells into less aggressive phyllodes lesions with mostly stromal tissue. Surprisingly, PE3KOT mice developed many more SRC-3+/AR-/Syp+ NETCs versus control TRAMP mice, indicating SRC-3 expression was retained in NETCs. In contrast, TRAMP mice with global SRC-3 knockout did not develop any NETC, indicating SRC-3 is required for developing NETC. Analysis of cell-differentiating markers revealed that these NETCs might not be derived from the mature AR-/Syp+ neuroendocrine cells or the AR+/Syp- luminal epithelial tumor cells. Instead, these NETCs might originate from the SV40-T/t-transformed intermediate/progenitor epithelial cells. In summary, SRC-3 is required for both AR+/Syp- AH tumor growth and AR-/Syp+ NETC development, suggesting SRC-3 is a target for inhibiting aggressive prostate cancer containing NETCs.

authors

• Wang, Fen

published proceedings

• Int J Biol Sci

author list (cited authors)

• Tien, J., Liao, L., Liu, Y., Liu, Z., Lee, D., Wang, F., & Xu, J.

citation count

• 10

complete list of authors

• Tien, Jean Ching-Yi||Liao, Lan||Liu, Yonghong||Liu, Zhaoliang||Lee, Dong-Kee||Wang, Fen||Xu, Jianming

publication date

• October 2014

publisher

• Ivyspring International Publisher  Publisher

published in

• International Journal of Biological Sciences  Journal

keywords

• Animals
• Carcinogenesis
• Coactivator
• Gene Knockout Techniques
• Histological Techniques
• Immunohistochemistry
• Male
• Mice
• Neuroendocrine Cell
• Neuroendocrine Tumors
• Nuclear Receptor Coactivator 3
• Prostate Epithelium
• Prostatic Neoplasms
• Src-3/ncoa3
• Synaptophysin
• Transgenic Mouse Model.

PubMed Central ID

• 25332686

Digital Object Identifier (DOI)

• 10.7150/ijbs.10236

URI

• https://hdl.handle.net/1969.1/182824

start page

• 1116

end page

• 1127

volume

• 10

issue

• 10

URL

• http://dx.doi.org/10.7150/ijbs.10236