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首页> 外文期刊>Cancer Medicine >LncRNA PITPNA‐AS1 boosts the proliferation and migration of lung squamous cell carcinoma cells by recruiting TAF15 to stabilize HMGB3 mRNA
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LncRNA PITPNA‐AS1 boosts the proliferation and migration of lung squamous cell carcinoma cells by recruiting TAF15 to stabilize HMGB3 mRNA

机译:LNCRNA PITPNA-AS1通过募集TAF15稳定HMGB3 mRNA来促进肺鳞状细胞癌细胞的增殖和迁移

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摘要

Plenty of reports have probed the involvement of abnormally expressed lncRNAs in multiple cancers, including lung squamous cell carcinoma (LUSC). Through online database GEPIA, lncRNA PITPNA antisense RNA 1 (PITPNA‐AS1) was highly expressed in LUSC samples, and these tendency was further affirmed in LUSC cells. The aim of current study was to investigate the related mechanism of PITPNA‐AS1 in LUSC. Functional experiments verified that depletion of PITPNA‐AS1 hampered the proliferative and migratory abilities, but accelerated apoptosis of LUSC cells. Additionally, we observed the increased expression of HMGB3 and its positive correlation with PITPNA‐AS1 in LUSC samples. Interestingly, PITPNA‐AS1 mainly located in the cytosol of LUSC cells, and also affected mRNA stability of HMGB3. Furthermore, the repressed mRNA stability of HMGB3 by PITPNA‐AS1 via TAF15 was exposed through mechanism experiments. The mediatory function of PITPNA‐AS1 on HMGB3 was validated via rescue assays. All in all, PITPNA‐AS1 promoted the proliferation and migration of LUSC cells via stabilizing HMGB3 by TAF15. In conclusion, our study displayed a novel mechanism underlying PITPNA‐AS1 in LUSC cells.
机译:大量的报告探讨了异常表达的LNCRNA在多种癌症中的参与,包括肺鳞状细胞癌(LUSC)。通过在线数据库Gepia,LNCRNA pitPNA反义RNA 1(PITPNA-AS1)在LUSC样品中高度表达,并且在LUSC细胞中进一步肯定了这些趋势。目前研究的目的是探讨LUSC中PITPNA-AS1的相关机制。功能实验证实,PITPNA-AS1的耗尽阻碍了增殖性和迁移能力,但加速了LUSC细胞的凋亡。另外,我们观察到HMGB3的表达增加及其与LUSC样品中PITPNA-AS1的正相关。有趣的是,PITPNA-AS1主要位于LUSC细胞的细胞溶胶,并且还影响了HMGB3的mRNA稳定性。此外,通过TAF15将HMGB3的抑制mRNA稳定性通过TAF15通过机理实验曝光。通过救援测定验证了PITPNA-AS1对HMGB3的介质功能。总而言之,PITPNA-AS1通过TAF15通过稳定HMGB3促进LUSC细胞的增殖和迁移。总之,我们的研究显示了LUSC细胞中PITPNA-AS1的新机制。

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