Downregulation of Astrocyte Elevated Gene-1 Expression Combined with All-Trans Retinoic Acid Inhibits Development of Vasculogenic Mimicry and Angiogenesis in Glioma

Objective This study aimed to investigate the effects of downregulating astrocyte elevated gene-1(AEG-1)expression combined with all-trans retinoic acid(ATRA)on vasculogenic mimicry(VM)formation and angiogenesis in glioma.Methods U87 glioma cells were transfected with AEG-1 shRNA lentiviral vectors(U87-siAEG-1)and incubated in a medium containing 20µmol/L ATRA.Matrigel-based tube formation assay was performed to evaluate VM formation,and the cell counting kit-8(CCK-8)assay was used to analyze the proliferation of glioma cells in vitro.Reverse transcription-quantitative polymerase chain reaction and Western blot analysis were used to investigate the mRNA and protein expression of related genes,respectively.Glioma xenograft models were generated via subcutaneous implantation of glioma cells in nude mice.Tumor-bearing mice received an intraperitoneal injection of ATRA(10 mg/kg per day).Immunohistochemistry was used to evaluate the expression of related genes and the microvessel density(MVD)in glioma xenograft models.CD34/periodic acid-Schiff double staining was performed to detect VM channels in vivo.The volume and weight of tumors were measured,and a tumor growth curve was drawn to evaluate tumor growth.Results A combination of ATRA intervention and downregulation of AEG-1 expression significantly inhibited the proliferation of glioma cells in vitro and glioma VM formation in vitro and in vivo.It also significantly decreased MVD and inhibited tumor growth.Further,the expression levels of matrix metalloproteinase(MMP)-2,MMP-9,vascular endothelial-cadherin(VE-cadherin),and vascular endothelial growth factor(VEGF)in glioma significantly decreased in vivo and in vivo.Conclusion Hence,a combinatorial approach might be effective in treating glioma through regulating MMP-2,MMP-9,VEGF,and VE-cadherin expression.

凋亡蛋白酶活化因子-1和星形细胞上调基因-1在胃癌中的表达及临床意义

目的探讨凋亡蛋白酶活化因子-1(Apaf-1)和星形细胞上调基因-1(AEG-1)在胃癌中的表达及临床意义。方法选取2015年9月至2017年12月于新余市人民医院行胃癌切除术及病理证实的50例胃癌患者的胃癌组织和癌旁组织标本,采用免疫组化法测定胃癌及癌旁组织中Apaf-1、AEG-1表达水平,分析Apaf-1、AEG-1表达水平与胃癌患者临床病理特征的关系及Apaf-1与AEG-1表达水平的相关性。结果癌旁组织中Apaf-1阳性表达率(78.00%)高于胃癌组织(20.00%),胃癌组织中AEG-1阳性表达率(82.00%)明显高于癌旁组织(26.00%),差异有统计学意义(P<0.05)。胃癌组织中Apaf-1、AEG-1表达水平均与肿瘤分化程度、浸润深度、TNM分期及淋巴结转移有关(P<0.05),与性别、年龄、肿瘤大小、肿瘤部位无关;经Spearman相关性分析结果显示,胃癌组织中Apaf-1表达水平与AEG-1表达水平呈显著负相关(r<0,P<0.05)。结论胃癌组织中AEG-1呈高表达,Apaf-1呈低表达,二者与胃癌的疾病进展密切相关,Apaf-1和AEG-1的肿瘤基因检测可能成为治疗胃癌的新靶点,具有较高的研究价值。

Astrocyte elevated gene-1 induces breast cancer proliferation and invasion through upregulating HER2/neu expression

Background Astrocyte elevated gene-1 （AEG-1）, primarily identified as a late response gene induced by HIV-1 infection, plays multiple roles in the process of oncogenesis. This novel gene has been demonstrated to be involved in the several potent carcinogenic pathways, including PI3K/Akt pathway, nuclear factor （NF）-KB pathway, and Wnt/13-catenin pathway. Although the function of AEG-1 has been intensively investigated in recent years, the molecular mechanism underlying its oncogenic role is largely unknown. The aim of this research was to explore the potential function of AEG-1 in breast cancer development and progression. Methods AEG-1 was ectopically overexpressed in breast cancer MCF-7 cells and its biological effects on the proliferation and invasion of MCF-7 cells were studied by 3-（4,5-dimethylthiazol-2-yl）-2,5-diphenyltetrazolium bromide （MTT） and invasion assays. The expression of HER2/neu, a crucial oncogene involving in breast cancer carcinogenesis, was also determined. Results Overexpression of the AEG-1 promoted the proliferation and invasion ability of breast cancer cells, and upregulated the expression of HER2/neu, a crucial oncogene involving in breast cancer carcinogenesis. Conclusion AEG-1 might facilitate the proliferation and invasion of breast cancer cells by upregulating HER2/neu expression, which provides a potential target for breast cancer therapy.

Metadherin-driven promotion of cancer stem cell phenotypes and its effect on immunity in hepatocellular carcinoma

In this editorial we provide commentary on the article published by Wang et al,featured in the recent issue of the World Journal of Gastroenterology in 2024.We focus on the metadherin(MTDH),also known as astrocyte elevated gene-1 or lysine rich CEACAM1,and its effects on cancer stem cells(CSCs)and immunity in hepatocellular carcinoma(HCC).HCC is the most common primary liver cancer and one of the leading causes of cancer-related deaths worldwide.Most HCC cases develop in the context of liver cirrhosis.Among the pivotal mechanisms of carcinogenesis are gene mutations,dysregulation of diverse signaling pathways,epigenetic alterations,hepatitis B virus-induced hepatocarcinogenesis,chronic inflammation,impact of tumor microenvironment,oxidative stress.Over the years,extensive research has been conducted on the MTDH role in various tumor pathologies,such as lung,breast,ovarian,gastric,hepatocellular,colorectal,renal carcinoma,neuroblastoma,melanoma,and leukemias.Specifically,its involvement in tumor development processes including transformation,apoptosis evasion,angiogenesis,invasion,and metastasis via multiple signaling pathways.It has been demonstrated that knockdown or knockout of MTDH disrupt tumor development and metastasis.In addition,numerous reports have been carried out regarding the MTDH influence on HCC,demonstrating its role as a predictor of poor prognosis,aggressive tumor phenotypes prone to metastasis and recurrence,and exhibiting significant potential for therapy resistance.Finally,more studies finely investigated the influence of MTDH on CSCs.The CSCs are a small subpopulation of tumor cells that sharing traits with normal stem cells like self-renewal and differentiation abilities,alongside a high plasticity that alters their phenotype.Beyond their presumed role in tumor initiation,they can drive also disease relapse,metastasis,and resistance to chemo and radiotherapy.

AEG-1 participates in high glucose-induced activation of Rho kinase and epithelial-mesenchymal transition in proximal tubular epithelial cells

Objective:To prove whether astrocyte elevated gene-1(AEG-1) plays a role in high glucosestimulated Rho kinase activation and epithelial-mesenchymal transition(EMT) in human renal tubular epithelial(HK-2) cells.Methods:The protein levels of AEG-1,alpha-smooth muscle actin,E-cadherin and MYPT1 were determined by Western blot.Results:AEG-1 protein level was upregulated in HK-2 cells stimulated with high glucose.AEG-1 siRNA downregulated Rho kinase protein expression and blocked high glucose-induced EMT.Conclusions:Our results show that AEG-1 acts a key role in high glucoseinduced activation of Rho kinase and EMT in HK-2 cells.

AEG-1在5-氟尿嘧啶诱导的人口腔鳞状细胞癌细胞耐药中的作用

目的:探讨星形胶质细胞升高基因-1(astrocyte elevated gene-1,AEG-1)对5-氟尿嘧啶(5-FU)诱导的口腔鳞状细胞癌(oral squamous cell carcinoma,OSCC)细胞系耐药性的影响。方法:验证高(SCC15)、中(转染空质粒的对照组SCC15、CAL27)、低(CAL27)四组不同AEG-1表达量细胞模型AEG-1基因转染效果。MTT实验观察四组细胞对5-FU耐受性的变化;蛋白质印迹法和细胞划痕实验观察四组细胞在5-FU作用下caspase-3、MMP-2、MMP-9蛋白表达水平变化及细胞迁移能力的变化。结果:AEG-1基因在细胞中转染成功。MTT实验显示不同浓度5-FU作用四组细胞后,过表达组细胞的半数抑制浓度(IC50)为423.7μg/ml,其对照组为213.5μg/ml(P<0.05);沉默细胞组IC50值为291.6μg/ml,其对照组为463.1μg/ml(P<0.05)。Western blot显示过表达组及其对照组中5-FU的浓度分别为400μg/ml和200μg/ml时,MMP-2、MMP-9及caspase-3的表达水平开始升高(P<0.05);沉默组及其对照组中5-FU的浓度分别为240μg/ml和480μg/ml时,MMP-2、MMP-9及caspase-3的表达水平开始升高(P<0.05)。划痕实验显示加入相同浓度5-FU后过表达组细胞迁移率明显高于其对照组(P<0.05);而沉默组细胞迁移率明显低于其对照组(P<0.05)。结论:上调/下调AEG-1表达能增加/降低OSCC细胞对5-FU的耐药性,提示OSCC细胞的耐药性可能与AEG-1表达量相关,OSCC细胞系中AEG-1的表达情况可能能间接干扰临床药物化疗的效果。

宫颈癌组织中AEG-1和TLR3表达与其微血管密度及预后的相关性

目的探讨宫颈癌组织中星形细胞上调基因(AEG)-1、Toll样受体(TLRs)3表达与其微血管密度(MVD)及预后的相关性。方法选取2011年12月至2014年12月收治的112例宫颈癌患者为观察组(取其宫颈癌病灶标本),另选子宫肌瘤切除术患者74例为对照组(取其正常宫颈组织标本),对比两种组织AEG-1、TLR3表达水平及MVD,Pearson分析AEG-1、TLR3表达与MVD的相关性;分析宫颈癌预后影响因素,对比不同预后患者AEG-1、TLR3表达水平;Spearman分析宫颈癌组织中AEG-1、TLR3表达与预后影响因素的相关性;以宫颈癌组织中AEG-1、TLR3表达量均数划分为高表达者与低表达者,用直接计算法计算并对比不同AEG-1、TLR3表达者5年生存率。结果观察组AEG-1表达水平和MVD高于对照组,TLR3表达水平低于对照组(P均<0.01)。宫颈癌组织中AEG-1表达与MVD呈正相关关系(r=0.607,P<0.05),TLR3表达与MVD呈负相关关系(r=-0.466,P<0.05)。病理分期、淋巴结转移、分化程度、肿瘤直径是宫颈癌预后重要影响因素(P<0.05,P<0.01);AEG-1与病理分期、淋巴结转移、肿瘤直径呈正相关,与分化程度呈负相关(P均<0.01);TLR3与病理分期、淋巴结转移、肿瘤直径呈负相关,与分化程度呈正相关(P均<0.01)。AEG-1高表达者5年生存率低于低表达者(57.97%vs93.02%,χ^2=15.949,P<0.01);TLR3高表达者5年生存率高于低表达者(95.12%vs57.75%,χ^2=17.791,P<0.01)。结论宫颈癌组织中AEG-1表达与肿瘤MVD呈正相关,TLR3表达与MVD呈负相关,二者均参与肿瘤侵袭、转移过程,可作为评价宫颈癌预后的重要指标。

Inhibition of osteosarcoma growth and metastasis using a polysaccharide derivative of Amy-g-PLLD for the delivery of AEG-1 siRNA

Osteosarcoma is the most common primary malignant neoplasm of the bone in children and adolescents and has a high risk of relapse and metastasis. Of the various methods to treat osteosarcoma, the use of genetic approaches to inhibit the rapid growth of osteosarcoma while limiting tumor metastasis has presented a challenge in its implementation. Here, we successfully synthesized a polysaccharide derivative （Amy-g-PLLD） for delivery of astrocyte elevated gene-1 （AEG-1） small-interfering RNA （siRNA） （siAEG-1）, and used it for the first time to suppress osteosarcoma tumors in vitro and in vivo. Amy-g-PLLD/ siAEG-1 complexes were delivered into 143B human osteosarcoma cells with low resultant cytotoxicity. Osteosarcoma tumor proliferation and invasion were inhibited in vitro. Intratumoral injection of Amy-g-PLLD/siAEG-1 complexes markedly inhibited tumor growth and lung metastasis in 143B tumor-bearing mice. This biocompatible and effective approach employing a natural material- siRNA complex should pave the way for more genetic research in treating osteosarcoma.