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Long Non-coding RNA CBR3 Antisense RNA 1 is Downregulated in Colorectal Cancer and Inhibits miR-29a-Mediated Cell Migration and Invasion

机译:长链非编码 RNA CBR3 反义 RNA 1 在结直肠癌中下调并抑制 miR-29a 介导的细胞迁移和侵袭

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Although CBR3 Antisense RNA 1 (CBR3-AS1) has been characterized as an oncogenic long non-coding RNA (lncRNA) in several cancers, a recent study reported the downregulation of CBR3-AS1 in colorectal cancer (CRC). Therefore, we analyzed its role in CRC. CBR3-AS1 and microRNA-29a (miR-29a) expression in tissue samples from CRC patients were analyzed by RT-qPCR. The interaction between CBR3-AS1 and miR-29a was predicted by IntaRNA and validated by RNA pull-down assay. The location of CBR3-AS1 was analyzed by nuclear fractionation assay. CBR3-AS1 overexpression was performed to analyze its role in miR-29a expression. The roles of CBR3-AS1 and miR-29a in CRC cell migration and invasion were analyzed by Transwell assay. CBR3-AS1 was downregulated, and miR-29a was upregulated in CRC. CBR3-AS1 and miR-29a directly interacted with each other. CBR3-AS1 was localized in both nucleus and cytoplasm fractions. CBR3-AS1 overexpression failed to alter miR-29a expression but reduced its enhancing effects on cell invasion and migration. CBR3-AS1 is downregulated in CRC and inhibits miR-29a-mediated cell migration and invasion by sponging miR-29a.
机译:尽管 CBR3 反义 RNA 1 (CBR3-AS1) 在几种癌症中已被表征为致癌长链非编码 RNA (lncRNA),但最近的一项研究报道了结直肠癌 (CRC) 中 CBR3-AS1 的下调。因此,我们分析了它在CRC中的作用。RT-qPCR分析CRC患者组织样本中CBR3-AS1和microRNA-29a(miR-29a)的表达。通过IntaRNA预测CBR3-AS1和miR-29a之间的相互作用,并通过RNA下拉试验进行验证。通过核分离试验分析CBR3-AS1的位置。CBR3-AS1过表达分析其在miR-29a表达中的作用。通过Transwell法分析了CBR3-AS1和miR-29a在CRC细胞迁移和侵袭中的作用。在CRC中,CBR3-AS1下调,miR-29a上调。CBR3-AS1和miR-29a直接相互作用。CBR3-AS1 定位于细胞核和细胞质组分中。CBR3-AS1过表达未能改变miR-29a的表达,但降低了其对细胞侵袭和迁移的增强作用。CBR3-AS1 在 CRC 中下调,并通过海绵化 miR-29a 抑制 miR-29a 介导的细胞迁移和侵袭。

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