DLX5通过激活NOTCH信号通路促进骨肉瘤进展。
DLX5 promotes osteosarcoma progression via activation of the NOTCH signaling pathway.
作者信息
Zhang Xiaojing, Bian Huiqin, Wei Wei, Wang Qian, Chen Jinnan, Hei Ruoxuan, Chen Chen, Wu Xuan, Yuan Haochun, Gu Junxia, Lu Yaojuan, Cai Cheguo, Zheng Qiping
机构信息
Department of Hematological Laboratory Science, Jiangsu Key Laboratory of Medical Science and Laboratory Medicine, School of Medicine, Jiangsu University Zhenjiang 212013, China.
Shenzhen Academy of Peptide Targeting Technology at Pingshan, and Shenzhen Tyercan Bio-Pharm Co., Ltd. Shenzhen 518118, China.
出版信息
Am J Cancer Res. 2021 Jun 15;11(6):3354-3374. eCollection 2021.
The distal-less (dlx) homeobox transcription factors have been implicated roles in bone development. DLX5, in particular, was shown to play essential roles in osteoblast differentiation by targeting RUNX2, a master transcription factor for bone development. Interestingly, DLX5 has also been shown to play an oncogenic role in lung and other cancers, possibly via regulation of MYC expression. Given its dual roles in bone and cancer, this study aimed to investigate the effect of DLX5 on progression of osteosarcoma (OS), the primary bone cancer that is characterized by abnormal bone formation and osteoblast activity. Expression of DLX5 in OS cell lines was detected by quantitative real-time PCR (qRT-PCR) and western blot (WB). In vitro and in vivo assays were performed to investigate the oncogenic function of DLX5 in OS cells and xenograft models. Luciferase reporter assay was performed to determine the underlying mechanism of DLX5-mediated OS aggressiveness. The results showed that DLX5 was differentially expressed in OS cell lines, with significantly upregulated levels in HOS and MG-63 and relatively low levels in U2OS and 143B cell lines, compared with the normal bone cell line. DLX5 knockdown in HOS and MG-63 cell lines by siRNA inhibited OS cell growth and progression, and induced cell apoptosis and cell cycle changes both in vitro and in vivo. Meanwhile, DLX5 overexpression had the opposite effect on U2OS and 143B cell lines. Notably, a positive correlation between the expression patterns of NOTCH1 and DLX5 was also observed. The expression levels of NICD (NOTCH1 intracellular domain) and HES1 (classical target of NOTCH) were closely associated with DLX5 expression. Whereas knockdown of DLX5 in OS cells resulted in decreased expression of NOTCH1 and reduced cell proliferation and migration, which were rescued by overexpression of NOTCH1. We further analyzed DLX5 and NOTCH1 genes using JASPAR software and found two potential DLX5 binding sites within the promoter. Dual-luciferase assay demonstrated that DLX5 specifically activates the NOTCH1 promoter and controls its expression. Taken together, our results support that DLX5 plays an oncogenic role in OS development, which can at least partially, be attributed to activation of the NOTCH signaling pathway.
远端缺失(dlx)同源盒转录因子与骨骼发育有关。特别是DLX5,通过靶向RUNX2(一种骨骼发育的主要转录因子),在成骨细胞分化中发挥重要作用。有趣的是,DLX5在肺癌和其他癌症中也显示出致癌作用,可能是通过调节MYC表达。鉴于其在骨骼和癌症中的双重作用,本研究旨在探讨DLX5对骨肉瘤(OS)进展的影响,骨肉瘤是一种以异常骨形成和成骨细胞活性为特征的原发性骨癌。通过定量实时PCR(qRT-PCR)和蛋白质免疫印迹(WB)检测DLX5在OS细胞系中的表达。进行体外和体内实验,以研究DLX5在OS细胞和异种移植模型中的致癌功能。进行荧光素酶报告基因测定以确定DLX5介导的OS侵袭性的潜在机制。结果表明,与正常骨细胞系相比,DLX5在OS细胞系中差异表达,在HOS和MG-63中水平显著上调,在U2OS和143B细胞系中水平相对较低。通过siRNA敲低HOS和MG-63细胞系中的DLX5可抑制OS细胞生长和进展,并在体外和体内诱导细胞凋亡和细胞周期变化。同时,DLX5过表达对U2OS和143B细胞系有相反的作用。值得注意的是,还观察到NOTCH1和DLX5表达模式之间呈正相关。NICD(NOTCH1细胞内结构域)和HES1(NOTCH的经典靶点)的表达水平与DLX5表达密切相关。而在OS细胞中敲低DLX5导致NOTCH1表达降低,细胞增殖和迁移减少,而NOTCH1过表达可挽救这些变化。我们使用JASPAR软件进一步分析DLX5和NOTCH1基因,发现在启动子内有两个潜在的DLX5结合位点。双荧光素酶测定表明,DLX5特异性激活NOTCH1启动子并控制其表达。综上所述,我们的结果支持DLX5在OS发展中起致癌作用,这至少部分可归因于NOTCH信号通路的激活。
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