Abstract
BackgroundSAG (Sensitive to Apoptosis Gene), also known as RBX2, ROC2 or RNF7, is a RING component of CRL (Cullin-RING ligase), required for its activity. Our recent study showed that SAG/RBX2 co-operated with Kras to promote lung tumorigenesis, but antagonized Kras to inhibit skin tumorigenesis, suggesting a tissue/context dependent function of Sag. However, it is totally unknown whether and how Sag would play in prostate tumorigenesis, triggered by Pten loss.Methods Sag and Pten double conditional knockout mice were generated and prostate specific deletion of Sag and Pten was achieved by PB4-Cre, and their effect on prostate tumorigenesis was evaluated by H&E staining. The methods of immunohistochemistry (IHC) staining and Western blotting were utilized to examine expression of various proteins in prostate cancer tissues or cell lines. The effect of SAG knockdown in proliferation, survival and migration was evaluated in two prostate cancer cell lines. The poly-ubiquitylation of PHLPP1 and DEPTOR was evaluated by both in vivo and in vitro ubiquitylation assays.ResultsSAG is overexpressed progressively from early-to-late stage of human prostate cancer with the highest expression seen in metastatic lesion. Sag deletion inhibits prostate tumorigenesis triggered by Pten loss in a mouse model as a result of suppressed proliferation. SAG knockdown in human prostate cancer cells inhibits a) proliferation in monolayer and soft agar, b) clonogenic survival, and c) migration. SAG is an E3 ligase that promotes ubiquitylation and degradation of PHLPP1 and DEPTOR, leading to activation of the PI3K/AKT/mTOR axis, whereas SAG knockdown caused their accumulation. Importantly, growth suppression triggered by SAG knockdown was partially rescued by simultaneous knockdown of PHLPP1 or DEPTOR, suggesting their causal role. Accumulation of Phlpp1 and Deptor with corresponding inactivation of Akt/mTOR was also detected in Sag-null prostate cancer tissues.Conclusions Sag is an oncogenic cooperator of Pten-loss for prostate tumorigenesis. Targeting SAG E3 ligase may, therefore, have therapeutic value for the treatment of prostate cancer associated with Pten loss.Electronic supplementary materialThe online version of this article (doi:10.1186/s12943-016-0567-6) contains supplementary material, which is available to authorized users.
Highlights
SAG (Sensitive to Apoptosis Gene), known as RBX2, ROC2 or RNF7, is a RING component of CRL (Cullin-RING ligase), required for its activity
SAG is overexpressed in human prostate cancer tissues, whereas Sag prostate knockout inhibits tumorigenesis induced by Pten loss due to reduced proliferation Our recent study showed that both RBX1 and SAG/RBX2 are overexpressed in human non-small cell lung carcinomas [23, 44]
We found that MLN4924, a small molecule inhibitor of NEDD8 activating enzyme, which indirectly inhibits CRL E3 ubiquitin ligase by blocking cullin neddylation [15, 46], effectively extended the protein half-life of PHLPP1 and DEPTOR in DU145 (Additional file 1: Figure S4B) and PC3 cells (Additional file 1: Figure S4C)
Summary
SAG (Sensitive to Apoptosis Gene), known as RBX2, ROC2 or RNF7, is a RING component of CRL (Cullin-RING ligase), required for its activity. Prostate cancer is one of the most common malignancies and the second leading cause of cancer death in males [1]. It develops through successive stages including intraepithelial neoplasia (PIN), carcinoma in situ, invasive adenocarcinoma, and metastatic diseases [2]. While Sag deletion in the lung significantly reduced lung tumorigenesis [25], it accelerated skin tumorigenesis when deleted in the skin [29] It is unknown whether Sag plays a role in prostate tumorigenesis, and, if so, what is the underlying mechanism
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