雄激素受体 (AR) 信号通过调节 AKT→NF-κB→CXCL5 信号促进内皮细胞增殖和募集,从而促进 RCC 的进展。
Androgen receptor (AR) signaling promotes RCC progression via increased endothelial cell proliferation and recruitment by modulating AKT → NF-κB → CXCL5 signaling.
机构信息
Department of Urology, The First Affiliated Hospital, Xi'an Jiaotong University, Xi'an 710061, China.
Core Facility for Protein Research, Institute of Biophysics, Chinese Academy of Sciences, Beijing 100101, China.
出版信息
Sci Rep. 2016 Nov 16;6:37085. doi: 10.1038/srep37085.
Androgen receptor (AR) signaling may promote renal cell carcinoma (RCC) progression via altered HIF-2α/VEGF signaling. However, it remains unclear whether AR signaling also promotes RCC progression by recruiting vascular endothelial cells (ECs), key players in the development of blood vessels. In our study, AR increased EC proliferation and recruitment to the tumor microenvironment and promoted RCC progression. Mechanistically, AR modulated cytokine CXCL5 expression by altering AKT → NF-κB signaling, and interruption of AKT → NF-κB → CXCL5 signaling using either specific inhibitors or siRNA suppressed AR-enhanced EC recruitment and AR-EC-promoted RCC progression. The results obtained using an in vivo mouse model and a human clinical sample survey confirmed the role of AR in promoting RCC progression through enhancement of EC proliferation and/or recruitment via altered AKT → NF-κB → CXCL5 signaling. Targeting this newly identified AR-induced AKT → NF-κB → CXCL5 pathway may facilitate the development of new therapies for slowing RCC progression.
雄激素受体 (AR) 信号可能通过改变 HIF-2α/VEGF 信号促进肾细胞癌 (RCC) 的进展。然而,AR 信号是否也通过招募血管内皮细胞 (ECs) 促进 RCC 进展,ECs 是血管发育的关键参与者,目前尚不清楚。在我们的研究中,AR 增加了 EC 的增殖和对肿瘤微环境的募集,并促进了 RCC 的进展。从机制上讲,AR 通过改变 AKT→NF-κB 信号来调节细胞因子 CXCL5 的表达,并且使用特异性抑制剂或 siRNA 阻断 AKT→NF-κB→CXCL5 信号,可抑制 AR 增强的 EC 募集和 AR-EC 促进的 RCC 进展。使用体内小鼠模型和人类临床样本调查获得的结果证实了 AR 通过改变 AKT→NF-κB→CXCL5 信号促进 EC 增殖和/或募集来促进 RCC 进展的作用。靶向这个新确定的 AR 诱导的 AKT→NF-κB→CXCL5 通路可能有助于开发减缓 RCC 进展的新疗法。
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