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Tumor‐suppressive microRNA‐223 inhibits cancer cell migration and invasion by targeting ITGA3/ITGB1 signaling in prostate cancer

机译:肿瘤抑制性microRNA-223通过靶向前列腺癌中的ITGA3 / ITGB1信号传导来抑制癌细胞的迁移和侵袭

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Analysis of microRNA (miRNA) expression signatures in prostate cancer (PCa) and castration-resistant PCa has revealed that miRNA-223 is significantly downregulated in cancer tissues, suggesting that miR-223 acts as a tumor-suppressive miRNA by targeting oncogenes. The aim of this study was to investigate the functional roles of miR-223 and identify downstream oncogenic targets regulated by miR-223 in PCa cells. Functional studies of miR-223 were carried out to investigate cell proliferation, migration, and invasion using PC3 and PC3M PCa cell lines. Restoration of miR-223 significantly inhibited cancer cell migration and invasion in PCa cells. In silico database and genome-wide gene expression analyses revealed that ITGA3 and ITGB1 were direct targets of miR-223 regulation. Knockdown of ITGA3 and ITGB1 significantly inhibited cancer cell migration and invasion in PCa cells by regulating downstream signaling. Moreover, overexpression of ITGA3 and ITGB1 was observed in PCa clinical specimens. Thus, our data indicated that downregulation of miR-223 enhanced ITGA3/ITGB1 signaling and contributed to cancer cell migration and invasion in PCa cells. Elucidation of the molecular pathways modulated by tumor-suppressive miRNAs provides insights into the mechanisms of PCa progression and metastasis.
机译:对前列腺癌(PCa)和去势抵抗性PCa中的microRNA(miRNA)表达特征进行分析后发现,miRNA-223在癌组织中显着下调,这表明miR-223通过靶向癌基因而起抑癌作用。这项研究的目的是调查miR-223的功能作用,并鉴定mia-223在PCa细胞中调控的下游致癌靶标。使用PC3和PC3M PCa细胞系进行了miR-223的功能研究,以研究细胞的增殖,迁移和侵袭。 miR-223的恢复显着抑制PCa细胞中的癌细胞迁移和侵袭。在计算机数据库和全基因组基因表达分析中发现,ITGA3和ITGB1是miR-223调控的直接靶标。通过调节下游信号传导,抑制ITGA3和ITGB1可以显着抑制PCa细胞中的癌细胞迁移和侵袭。此外,在PCa临床标本中观察到ITGA3和ITGB1的过表达。因此,我们的数据表明,miR-223的下调增强了ITGA3 / ITGB1信号传导,并有助于癌细胞迁移和侵袭PCa细胞。肿瘤抑制性miRNA调控的分子途径的阐明提供了对PCa进展和转移机制的见解。

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