Differential requirements of androgen receptor in luminal progenitors during prostate regeneration and tumor initiation
| Autor: | Michael M. Shen, Hanina Hibshoosh, Antonina Mitrofanova, Bo I. Li, Chee Wai Chua, Eva Leung, Nusrat J. Epsi, Ming Lei, Sarah K. Bergren, Shouhong Xuan |
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| Jazyk: | angličtina |
| Rok vydání: | 2018 |
| Předmět: |
Male
0301 basic medicine Mouse Carcinogenesis QH301-705.5 Science Tumor initiation Biology medicine.disease_cause Neuroendocrine differentiation General Biochemistry Genetics and Molecular Biology Animals Genetically Modified Mice 03 medical and health sciences Prostate cancer androgen receptor medicine Animals Regeneration PTEN mouse models Progenitor cell Biology (General) Cancer Biology Cell Proliferation prostate General Immunology and Microbiology General Neuroscience Epithelial Cells progenitor General Medicine cell of origin medicine.disease 3. Good health Androgen receptor Developmental Biology and Stem Cells 030104 developmental biology Receptors Androgen Cancer research biology.protein Medicine Stem cell Research Article Human |
| Zdroj: | eLife, Vol 7 (2018) eLife |
| Popis: | Master regulatory genes of tissue specification play key roles in stem/progenitor cells and are often important in cancer. In the prostate, androgen receptor (AR) is a master regulator essential for development and tumorigenesis, but its specific functions in prostate stem/progenitor cells have not been elucidated. We have investigated AR function in CARNs (CAstration-Resistant Nkx3.1-expressing cells), a luminal stem/progenitor cell that functions in prostate regeneration. Using genetically--engineered mouse models and novel prostate epithelial cell lines, we find that progenitor properties of CARNs are largely unaffected by AR deletion, apart from decreased proliferation in vivo. Furthermore, AR loss suppresses tumor formation after deletion of the Pten tumor suppressor in CARNs; however, combined Pten deletion and activation of oncogenic Kras in AR-deleted CARNs result in tumors with focal neuroendocrine differentiation. Our findings show that AR modulates specific progenitor properties of CARNs, including their ability to serve as a cell of origin for prostate cancer. eLife digest Most prostate tumors rely on male hormones – called androgens – to survive. Aggressive prostate cancer is often treated with drugs that block androgens, which usually cause the prostate tumors to shrink. One class of the drugs works by binding to and inactivating the androgen receptor protein on prostate cancer cells. However, aggressive prostate tumors can often become resistant to these anti-androgen therapies. It is not clear where the resistant cancer cells come from. In 2009, researchers showed that the normal prostate contains some cells that appear to be independent of androgens. A subset of these cells – also known as CARNs – can act as stem or progenitor cells that can repair the prostate after injury. These normal androgen-independent cells can also be the cells from which prostate tumors arise. Here, Chua et al. – including one of the researchers from the 2009 study – investigated how these CARN cells behave when the androgen receptor is deleted. When the androgen receptor was genetically removed in CARN cells of otherwise healthy mice, the behavior of CARN cells was unaffected. When the androgen receptor was deleted together with a protein that normally suppresses the formation of tumors, it protected the mice from prostate cancer. However, Chua et al. also observed that deleting the androgen receptor could not prevent the tumor from growing when two cancer-causing mutations were present. These tumors were similar to human prostate tumors that are resistant to anti-androgen therapy. Since CARN cells may also exist in humans, this new way of making prostate cancers in mice may be used to study how these resistances arise in patients. A better understanding of how prostate tumors develop might lead to new treatments in which the androgen receptor is blocked in combination with other new protein targets. |
| Databáze: | OpenAIRE |
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