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首页> 外文期刊>Biochimica et biophysica acta. Molecular basis of disease: BBA >Down-regulated expression of LINC00518 prevents epithelial cell growth and metastasis in breast cancer through the inhibition of CDX2 methylation and the Wnt signaling pathway
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Down-regulated expression of LINC00518 prevents epithelial cell growth and metastasis in breast cancer through the inhibition of CDX2 methylation and the Wnt signaling pathway

机译:LINC00518的下调表达通过抑制CDX2甲基化和WNT信号通路来防止乳腺癌中皮细胞生长和转移

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Breast cancer (BC)-related mortality is associated with the potential metastatic properties of the primary breast tumors. The following study was conducted with the main focus on the effect of LINC00518 on the growth and metastasis of BC epithelial cells via the Wnt signaling pathway through regulation of the methylation of CDX2 gene. Initially, differentially expressed long intergenic non-protein coding RNAs (lincRNAs) related to BC were screened out in the Cancer Genome Atlas (TCGA) database, after which we detected the LINC00518 expression and localization in BC tissues and cells. Then the CDX2 positive expression and methylation level were identified. The targeting relationship of LINC00518 and CDX2, and binding methyltransferase in the promoter region were examined. BC epithelial cell proliferation, colony formation ability, invasion, migration and apoptosis were further evaluated. The lincRNA expression data related to BC downloaded from the TCGA database revealed that there was a high expression of LINC00518 in BC, and a negative correlation between LINC00518 and CDX2. In addition, LINC00518 promotes CDX2 methylation by recruiting DNA methyltransferase through activating the Wnt signaling pathway. The down-regulation of LINC00518 inhibited proliferation, invasion, migration, and EMT of BC epithelial cells while enhancing apoptosis. The inhibitory effects of LINC00518 down-regulation was reversed by CDX2 down-regulation. In conclusion, our findings revealed that down-regulation of LINC00518 might have the ability to suppress BC progression by up-regulating CDX2 expression through the reduction of methylation and blockade of the Wnt signaling pathway, resulting in the inhibition of proliferation and promotion of apoptosis of BC epithelial cells.
机译:乳腺癌(BC) - 相关的死亡率与原发性乳腺肿瘤的潜在转移性有关。通过主要重点关注LINC00518通过调节CDX2基因的甲基化通过Wnt信号通路对BC上皮细胞生长和转移的影响。最初,在癌症基因组Atlas(TCGA)数据库中筛选与BC相关的差异表达的长期非蛋白质编码RNA(LincrNA),之后我们在BC组织和细胞中检测到LINC00518的表达和定位。然后鉴定CDX2阳性表达和甲基化水平。研究了LINC00518和CDX2的靶向关系,并在启动子区中结合甲基转移酶。进一步评估了BC上皮细胞增殖,菌落形成能力,侵袭,迁移和细胞凋亡。与TCGA数据库下载的BC相关的LINCRNA表达数据显示在BC中存在LINC00518的高表达,以及LINC00518和CDX2之间的负相关。此外,通过激活Wnt信号通路募集DNA甲基转移酶,LINC00518通过激活WNT信号通路来促进CDX2甲基化。 LINC00518的下调抑制BC上皮细胞的增殖,侵袭,迁移和EMT,同时增强凋亡。通过CDX2下调逆转LINC00518下调的抑制作用。总之,我们的研究结果表明,LINC00518的下调可能通过降低甲基化和WNT信号传导途径的降低来抑制BC进展,导致抑制细胞凋亡和促进凋亡的抑制BC上皮细胞。

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