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Integration of regulatory networks by NKX3-1 promotes androgen-dependent prostate cancer survival
Tan P.Y.1; Chang C.W.1; Chng K.R.1; Senali Abayratna Wansa K.D.1; Sung W.-K.1; Cheung E.1
2012
Source PublicationMolecular and Cellular Biology
ISSN02707306 10985549
Volume32Issue:2Pages:399-414
Abstract

The NKX3-1 gene is a homeobox gene required for prostate tumor progression, but how it functions is unclear. Here, using chromatin immunoprecipitation coupled to massively parallel sequencing (ChIP-seq) we showed that NKX3-1 colocalizes with the androgen receptor (AR) across the prostate cancer genome. We uncovered two distinct mechanisms by which NKX3-1 controls the AR transcriptional network in prostate cancer. First, NKX3-1 and AR directly regulate each other in a feed-forward regulatory loop. Second, NKX3-1 collaborates with AR and FoxA1 to mediate genes in advanced and recurrent prostate carcinoma. NKX3-1- and AR-coregulated genes include those found in the "protein trafficking" process, which integrates oncogenic signaling pathways. Moreover, we demonstrate that NKX3-1, AR, and FoxA1 promote prostate cancer cell survival by directly upregulating RAB3B, a member of the RAB GTPase family. Finally, we show that RAB3B is overexpressed in prostate cancer patients, suggesting that RAB3B together with AR, FoxA1, and NKX3-1 are important regulators of prostate cancer progression. Collectively, our work highlights a novel hierarchical transcriptional regulatory network between NKX3-1, AR, and the RAB GTPase signaling pathway that is critical for the genetic-molecular-phenotypic paradigm in androgen-dependent prostate cancer. © 2012, American Society for Microbiology.

DOI10.1128/MCB.05958-11
URLView the original
Indexed BySCIE
WOS Research AreaBiochemistry & Molecular Biology ; Cell Biology
WOS SubjectBiochemistry & Molecular Biology ; Cell Biology
WOS IDWOS:000299020100014
Scopus ID2-s2.0-84863072810
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Citation statistics
Document TypeJournal article
CollectionFaculty of Health Sciences
Affiliation1.A-Star, Genome Institute of Singapore
2.Nanyang Technological University
3.National University of Singapore
4.Yong Loo Lin School of Medicine
Recommended Citation
GB/T 7714
Tan P.Y.,Chang C.W.,Chng K.R.,et al. Integration of regulatory networks by NKX3-1 promotes androgen-dependent prostate cancer survival[J]. Molecular and Cellular Biology, 2012, 32(2), 399-414.
APA Tan P.Y.., Chang C.W.., Chng K.R.., Senali Abayratna Wansa K.D.., Sung W.-K.., & Cheung E. (2012). Integration of regulatory networks by NKX3-1 promotes androgen-dependent prostate cancer survival. Molecular and Cellular Biology, 32(2), 399-414.
MLA Tan P.Y.,et al."Integration of regulatory networks by NKX3-1 promotes androgen-dependent prostate cancer survival".Molecular and Cellular Biology 32.2(2012):399-414.
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