Prostate cancer reactivates developmental epigenomic programs during metastatic progression
- Pomerantz, Mark M.
- Qiu, Xintao
- Zhu, Yanyun
- Takeda, David Y.
- Pan, Wenting
- Baca, Sylvan C.
- Gusev, Alexander
- Korthauer, Keegan D.
- Severson, Tesa M.
- Ha, Gavin
- Viswanathan, Srinivas R.
- Seo, Ji Heui
- Nguyen, Holly M.
- Zhang, Baohui
- Pasaniuc, Bogdan
- Giambartolomei, Claudia
- Alaiwi, Sarah A.
- Bell, Connor A.
- O’Connor, Edward P.
- Chabot, Matthew S.
- Stillman, David R.
- Lis, Rosina
- Font-Tello, Alba
- Li, Lewyn
- Cejas, Paloma
- Bergman, Andries M.
- Sanders, Joyce
- van der Poel, Henk G.
- Gayther, Simon A.
- Lawrenson, Kate
- Fonseca, Marcos A.S.
- Reddy, Jessica
- Corona, Rosario I.
- Martovetsky, Gleb
- Egan, Brian
- Choueiri, Toni
- Ellis, Leigh
- Garraway, Isla P.
- Lee, Gwo Shu Mary
- Corey, Eva
- Long, Henry W.
- Zwart, Wilbert
- Freedman, Matthew L.
DOIAbstract
Epigenetic processes govern prostate cancer (PCa) biology, as evidenced by the dependency of PCa cells on the androgen receptor (AR), a prostate master transcription factor. We generated 268 epigenomic datasets spanning two state transitions—from normal prostate epithelium to localized PCa to metastases—in specimens derived from human tissue. We discovered that reprogrammed AR sites in metastatic PCa are not created de novo; rather, they are prepopulated by the transcription factors FOXA1 and HOXB13 in normal prostate epithelium. Reprogrammed regulatory elements commissioned in metastatic disease hijack latent developmental programs, accessing sites that are implicated in prostate organogenesis. Analysis of reactivated regulatory elements e...
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