MEG3的缺失通过NQO1/FSCN1途径促进了砷诱导致癌过程中迁移和侵袭能力的增强。
Loss of MEG3 contributes to the enhanced migration and invasion in arsenic-induced carcinogenesis through NQO1/FSCN1 pathway.
作者信息
Tu Huailu, Zhang Zhuo, Li Jingxia, Shi Sophia, Costa Max
机构信息
Division of Environmental Medicine, Department of Medicine, New York University School of Medicine 341 E 25th Street, New York, NY 10010, USA.
出版信息
Am J Cancer Res. 2023 Jun 15;13(6):2307-2322. eCollection 2023.
Arsenic ranks at the top among all toxic metals and poses a serious threat to human health. Inorganic arsenite and arsenate compounds have been classified as human carcinogens in various types of cancers. Maternally expressed gene 3 (MEG3), a tumor suppressor that is commonly lost in cancer, was investigated in this study for its role in the migration and invasion of arsenic-transformed cells. Our results showed that MEG3 was downregulated in both arsenic-transformed cells (As-T) and cells treated with low doses of arsenic for three months (As-treated). The analysis using TCGA dataset revealed that MEG3 expression was significantly reduced in the tumor tissues from human lung adenocarcinoma (LUAD) and lung squamous cell carcinoma (LUSC) compared to normal lung tissues. The results from the methylation-specific PCR (MSP) assay demonstrated enhanced methylation in the MEG3 promoters in both As-T and As-treated cells, indicating that increased methylation of the MEG3 promoter caused MEG3 downregulation in these cells. Moreover, As-T cells displayed increased migration and invasion and higher levels of NAD(P)H quinone dehydrogenase 1 (NQO1) and fascin actin-bundling protein 1 (FSCN1). Consistently, the results from immunohistochemistry staining showed that both NQO1 and FSCN1 are highly expressed in human lung squamous cell carcinoma tissues compared to those in normal lungs. Knockdown of MEG3 in normal BEAS-2B cells also led to increased migration and invasion, along with elevated levels of NQO1 and FSCN1. The negative regulation of MEG3 on FSCN1 was restored by NQO1 overexpression in both As-T and BEAS-2B cells. The results from immunoprecipitation assays confirmed the direct binding of NQO1 to FSCN1. Overexpression of NQO1 increased migration and invasion abilities in BEAS-2B cells, while knockdown of NQO1 by its shRNA reduced these two hallmarks of cancer. Interestingly, the reduced migration and invasion by NQO1 knockdown were restored by FSCN1. Collectively, the loss of MEG3 upregulated NQO1, which in turn stabilized FSCN1 protein through its direct binding, resulting in elevated migration and invasion in arsenic-transformed cells.
砷在所有有毒金属中位列榜首,对人类健康构成严重威胁。无机亚砷酸盐和砷酸盐化合物已被归类为多种癌症的人类致癌物。母系表达基因3(MEG3)是一种在癌症中通常缺失的肿瘤抑制因子,本研究对其在砷转化细胞的迁移和侵袭中的作用进行了研究。我们的结果表明,MEG3在砷转化细胞(As-T)和用低剂量砷处理三个月的细胞(As-处理)中均下调。使用TCGA数据集进行的分析显示,与正常肺组织相比,人肺腺癌(LUAD)和肺鳞状细胞癌(LUSC)肿瘤组织中的MEG3表达显著降低。甲基化特异性PCR(MSP)检测结果表明,As-T细胞和As-处理细胞中MEG3启动子的甲基化增强,表明MEG3启动子甲基化增加导致这些细胞中MEG3下调。此外,As-T细胞表现出迁移和侵袭增加以及NAD(P)H醌脱氢酶1(NQO1)和肌动蛋白成束蛋白1(FSCN1)水平升高。一致地,免疫组织化学染色结果显示,与正常肺组织相比,NQO1和FSCN1在人肺鳞状细胞癌组织中均高表达。在正常BEAS-2B细胞中敲低MEG3也导致迁移和侵袭增加,同时NQO1和FSCN1水平升高。在As-T细胞和BEAS-2B细胞中,NQO1过表达恢复了MEG3对FSCN1的负调控。免疫沉淀检测结果证实了NQO1与FSCN1的直接结合。NQO1过表达增加了BEAS-2B细胞的迁移和侵袭能力,而用其shRNA敲低NQO1则降低了这两个癌症特征。有趣的是,FSCN1恢复了NQO1敲低导致的迁移和侵袭减少。总体而言,MEG3的缺失上调了NQO1,而NQO1又通过其直接结合稳定了FSCN1蛋白,导致砷转化细胞的迁移和侵袭增加。
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