| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 2107713 | Cancer Cell | 2010 | 16 Pages |
SummaryNeuroendocrine (NE) phenotype, seen in >30% of prostate adenocarcinomas (PCa), and NE prostate tumors are implicated in aggressive prostate cancer. Formation of NE prostate tumors in the TRAMP mouse model was suppressed in mice lacking the ubiquitin ligase Siah2, which regulates HIF-1α availability. Cooperation between HIF-1α and FoxA2, a transcription factor expressed in NE tissue, promotes recruitment of p300 to transactivate select HIF-regulated genes, Hes6, Sox9, and Jmjd1a. These HIF-regulated genes are highly expressed in metastatic PCa and required for hypoxia-mediated NE phenotype, metastasis in PCa, and the formation of NE tumors. Tissue-specific expression of FoxA2 combined with Siah2-dependent HIF-1α availability enables a transcriptional program required for NE prostate tumor development and NE phenotype in PCa.
► Ubiquitin ligase Siah2 is required for NE prostate tumor development ► HIF1α and FoxA2 cooperation identifies tissue-specific HIF transcriptional synergy ► HIF1α/FoxA2 target genes are required for NE phenotype of prostate tumors ► HIF1α/FoxA2 target genes are highly expressed in metastatic prostate tumors
