Abstract

BackgroundGrowth factors activating the ErbB receptors have been described in prostate tumors. The androgen dependent prostate cancer cell line, LNCaP, expresses the ErbB-1, ErbB-2 and ErbB-3 receptor tyrosine kinases. Previously, it was demonstrated that NRG activates ErbB-2/ErbB-3 heterodimers to induce LNCaP cell death, whereas, EGF activates ErbB-1/ErbB-1 or ErbB-1/ErbB-2 dimers to induce cell growth and survival. It was also demonstrated that PI3K inhibitors repressed this cell death suggesting that in androgen deprived LNCaP cells, NRG activates a PI3K-dependent pathway associated with cell death.Methodology/Principal FindingsIn the present study we demonstrate that NRG induces autophagy in LNCaP cells, using LC3 as a marker. However, the autophagy induced by NRG may be incomplete since p62 levels elevate. We also demonstrated that NRG- induced autophagy is independent of mammalian target of rapamycin (mTOR) inhibition since NRG induces Akt and S6K activation. Interestingly, inhibition of reactive oxygen species (ROS) by N-acetylcysteine (NAC), inhibited NRG-induced autophagy and cell death. Our study also identified JNK and Beclin 1 as important components in NRG-induced autophagy and cell death. NRG induced elevation in JNK phosphorylation that was inhibited by NAC. Moreover, inhibitor of JNK inhibited NRG-induced autophagy and cell death. Also, in cells overexpressing Bcl-2 or cells expressing sh-RNA against Beclin 1, the effects of NRG, namely induction of autophagy and cell death, were inhibited.Conclusions/SignificanceThus, in LNCaP cells, NRG-induces incomplete autophagy and cell death that depend on ROS levels. These effects of NRG are mediated by signaling pathway that activates JNK and Beclin 1, but is independent of mTOR inhibition.

Highlights

  • Prostatic carcinoma is one of the most common male cancers

  • We analyzed the effect of NRG on autophagy and cell death of LNCaP cells grown without androgen mimetic

  • To further explore the signaling pathway involved in NRG-induced autophagy in LNCaP cells, we examined the activation of Erk and JNK, two known mitogen activated protein kinases (MAPKs) which are downstream signaling components of ErbB receptors [39]

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Summary

Introduction

Prostatic carcinoma is one of the most common male cancers. Prostate cells growth is regulated by hormones, growth factors and their respective receptors. Among the most frequent group of receptors implicated in human cancers is the ErbB subfamily of receptor tyrosine kinases [1,2,3]. Whereas ErbB-1 receptor (known as epidermal growth factor receptor, EGFR), is activated by EGF and EGF-like ligands, ErbB-3 and ErbB-4 receptors are activated by NRG/neuregulin isoforms and ErbB-2 receptor has no known ligand [4]. The androgen dependent prostate cancer cell line, LNCaP, expresses the ErbB-1, ErbB-2 and ErbB-3 receptor tyrosine kinases. It was demonstrated that PI3K inhibitors repressed this cell death suggesting that in androgen deprived LNCaP cells, NRG activates a PI3K-dependent pathway associated with cell death

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