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LncRNA ROR1-AS1 accelerates osteosarcoma invasion and proliferation through modulating miR-504

机译:LNCRNA ROR1-AS1通过调制MIR-504加速骨肉瘤侵袭和增殖

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摘要

Long non-coding RNAs (LncRNAs) play vital roles in the progression and development of tumors. However, the functional role of ROR1-AS1 in osteosarcoma has not been investigated. We found that ROR1-AS1 was upregulated in osteosarcoma tissues compared to non-tumor samples. Elevated expression of ROR1-AS1 promoted cyclin D1, PCNA and ki-67 expression and increased cell cycle and growth in MG-63 cell. Moreover, overexpression of ROR1-AS1 induced cell migration in MG-63 cell, promoting N-cadherin and vimentin expression and inhibiting E-cadherin expression. Dual-luciferase assay proved that ROR1-AS1 served as one sponge for miR-504 and ROR1-AS1 overexpression suppressed miR-504 expression in MG-63 cell. ROR1-AS1 expression was lower in osteosarcoma tissues compared to non-tumor samples. Pearson's correlation assay showed a negative correlation between miR-504 and ROR1-AS1 expression. MiR-504 overexpression partly abrogated ROR1-AS1-induced effects on osteosarcoma cell migration and proliferation. These data implied that ROR1-AS1 played as an oncogene and might be a new treatment target for osteosarcoma.
机译:长期非编码RNA(LNCRNA)在肿瘤的进展和发展中起重要作用。然而,尚未研究ROR1-AS1在骨肉瘤中的功能作用。与非肿瘤样品相比,我们发现ROR1-AS1在骨肉瘤组织中上调。 ROR1-AS1的升高的表达促进了Cyclin D1,PCNA和Ki-67表达以及增加的细胞周期和Mg-63细胞的生长。此外,在Mg-63细胞中的ROR1-AS1诱导细胞迁移的过表达,促进N-CADHERIN和VIMENTIN表达并抑制E-Cadherin表达。双荧光素酶测定证明,ROR1-AS1用作MIR-504的一个海绵,ROR1-AS1过表达抑制MG-63细胞中的miR-504表达。与非肿瘤样品相比,骨肉瘤组织中的ROR1-AS1表达较低。 Pearson的相关测定显示MiR-504和ROR1-AS1表达之间的负相关性。 miR-504过表达部分废除了ROR1-AS1诱导的对骨肉瘤细胞迁移和增殖的影响。这些数据暗示ROR1-AS1作为癌基因发挥,并且可能是骨肉瘤的新治疗靶标。

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