TY - JOUR
T1 - Identification of a genetic interaction between the tumor suppressor EAF2 and the retinoblastoma protein (Rb) signaling pathway in C. Elegans and prostate cancer cells
AU - Cai, Liquan
AU - Wang, Dan
AU - Fisher, Alfred L.
AU - Wang, Zhou
N1 - Funding Information:
Wild type N2; MR142 (cdc-25.1(rr31) I; rrIs1(elt-2p:NLS-GFP); and DZ325 (ezIs2 III; him-8(e1489) IV, ezIs2[fkh-6::GFP + unc-119(+)]) were obtained from the C. elegans Genetics Center, which is supported in part by NIH funding. ALF50 (eaf-1(tm3976)) was described previously [1] . ZH231 unc-76(e911) V; enIs7 [Pced-1 ced-1::GFP + unc-76(+)] X [9] was generously provided by Zheng Zhou (Baylor College of Medicine, Houston, TX). The rrIs1(elt-2p:NLS-GFP) transgene in a wild-type background was generated by outcrossing MR142 with N2.
Funding Information:
We are grateful to Dr. Shohei Mitani (National BioResource Project) for providing the eaf-1(tm3976) mutant. This research is supported in part by United States-NIH R37 DK51193 and AUA foundation to Zhou Wang and ES017761 and AG044768 to Alfred L. Fisher as well as resources from the San Antonio GRECC of the South Texas VA Healthcare system, United States .
PY - 2014/5/2
Y1 - 2014/5/2
N2 - The tumor suppressor EAF2 is regulated by androgen signaling and associated with prostate cancer. While EAF2 and its partner ELL have been shown to be members of protein complexes involved in RNA polymerase II transcriptional elongation, the biologic roles for EAF2 especially with regards to the development of cancer remains poorly understood. We have previously identified the eaf-1 gene in Caenorhabditis elegans as the ortholog of EAF2, and shown that eaf-1 interacts with the ELL ortholog ell-1 to control development and fertility in worms. To identify genetic pathways that interact with eaf-1, we screened RNAi libraries consisting of transcription factors, phosphatases, and chromatin-modifying factors to identify genes which enhance the effects of eaf-1(tm3976) on fertility. From this screen, we identified lin-53, hmg-1.2, pha-4, ruvb-2 and set-6 as hits. LIN-53 is the C. Elegans ortholog of human retinoblastoma binding protein 4/7 (RBBP 4/7), which binds to the retinoblastoma protein and inhibits the Ras signaling pathway. We find that lin-53 showed a synthetic interaction with eaf-1(tm3976) where knockdown of lin-53 in an eaf-1(tm3976) mutant resulted in sterile worms. This phenotype may be due to cell death as the treated worms contain degenerated embryos with increased expression of the ced-1:GFP cell death marker. Further we find that the interaction between eaf-1 and lin-53/RBBP4/7 also exists in vertebrates, which is reflected by the formation of a protein complex between EAF2 and RBBP4/7. Finally, overexpression of either human EAF2 or RBBP4 in LNCaP cells induced the cell death while knockdown of EAF2 in LNCaP enhanced cell proliferation, indicating an important role of EAF2 in controlling the growth and survival of prostate cancer cells. Together these findings identify a novel physical and functional interaction between EAF2 and the Rb pathway.
AB - The tumor suppressor EAF2 is regulated by androgen signaling and associated with prostate cancer. While EAF2 and its partner ELL have been shown to be members of protein complexes involved in RNA polymerase II transcriptional elongation, the biologic roles for EAF2 especially with regards to the development of cancer remains poorly understood. We have previously identified the eaf-1 gene in Caenorhabditis elegans as the ortholog of EAF2, and shown that eaf-1 interacts with the ELL ortholog ell-1 to control development and fertility in worms. To identify genetic pathways that interact with eaf-1, we screened RNAi libraries consisting of transcription factors, phosphatases, and chromatin-modifying factors to identify genes which enhance the effects of eaf-1(tm3976) on fertility. From this screen, we identified lin-53, hmg-1.2, pha-4, ruvb-2 and set-6 as hits. LIN-53 is the C. Elegans ortholog of human retinoblastoma binding protein 4/7 (RBBP 4/7), which binds to the retinoblastoma protein and inhibits the Ras signaling pathway. We find that lin-53 showed a synthetic interaction with eaf-1(tm3976) where knockdown of lin-53 in an eaf-1(tm3976) mutant resulted in sterile worms. This phenotype may be due to cell death as the treated worms contain degenerated embryos with increased expression of the ced-1:GFP cell death marker. Further we find that the interaction between eaf-1 and lin-53/RBBP4/7 also exists in vertebrates, which is reflected by the formation of a protein complex between EAF2 and RBBP4/7. Finally, overexpression of either human EAF2 or RBBP4 in LNCaP cells induced the cell death while knockdown of EAF2 in LNCaP enhanced cell proliferation, indicating an important role of EAF2 in controlling the growth and survival of prostate cancer cells. Together these findings identify a novel physical and functional interaction between EAF2 and the Rb pathway.
KW - Apoptosis
KW - C. Elegans
KW - RNAi library screen
KW - Retinoblastoma protein
KW - The tumor suppressor EAF2
KW - lin-53
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UR - http://www.scopus.com/inward/citedby.url?scp=84899991081&partnerID=8YFLogxK
U2 - 10.1016/j.bbrc.2014.03.138
DO - 10.1016/j.bbrc.2014.03.138
M3 - Article
C2 - 24727455
AN - SCOPUS:84899991081
SN - 0006-291X
VL - 447
SP - 292
EP - 298
JO - Biochemical and Biophysical Research Communications
JF - Biochemical and Biophysical Research Communications
IS - 2
ER -