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环状 RNA DOCK1 通过 miR-339-3p/IGF1R 轴促进骨肉瘤的发生发展和顺铂耐药性。

CircDOCK1 promotes the tumorigenesis and cisplatin resistance of osteogenic sarcoma via the miR-339-3p/IGF1R axis.

机构信息

Department of Bone and Soft Tissue Tumor Surgery, Cancer Hospital of China Medical University, Liaoning Cancer Hospital & Institute, Shenyang, 110042, Liaoning Province, China.

出版信息

Mol Cancer. 2021 Dec 7;20(1):161. doi: 10.1186/s12943-021-01453-0.

Abstract

BACKGROUND

Circular RNAs (circRNAs), a class of noncoding RNAs (ncRNAs), may modulate gene expression by binding to miRNAs. Additionally, recent studies show that circRNAs participate in some pathological processes. However, there is a large gap in the knowledge about circDOCK1 expression and its biological functions in osteogenic sarcoma (OS).

METHODS

Differentially expressed circRNAs in OS cell lines and tissues were identified by circRNA microarray analysis and quantitative real-time PCR (qRT-PCR). To explore the actions of circDOCK1 in vivo and in vitro, circDOCK1 was knocked down or overexpressed. To assess the binding and regulatory associations among miR-339-3p, circDOCK1 and IGF1R, we performed rescue experiments, RNA immunoprecipitation (RIP), RNA pulldown assays and dual-luciferase assays. Moreover, we performed apoptosis assays to reveal the regulatory effects of the circDOCK1/miR-339-3p/IGF1R axis on cisplatin sensitivity.

RESULTS

CircDOCK1 expression remained stable in the cytoplasm and was higher in OS tissues and cells than in the corresponding controls. Overexpression of circDOCK1 increased oncogenicity in vivo and malignant transformation in vitro. In the U2OS and MG63 cell lines, circDOCK1 modulated tumor progression by regulating IGF1R through sponging of miR-339-3p. Additionally, in the U2OS/DDP and MG63/DDP cell lines, cisplatin sensitivity was regulated by circDOCK1 via the miR-339-3p/IGF1R axis.

CONCLUSIONS

CircDOCK1 can promote progression and regulate cisplatin sensitivity in OS via the miR-339-3p/IGF1R axis. Thus, the circDOCK1/miR-339-3p/IGF1R axis may be a key mechanism and therapeutic target in OS.

摘要

背景

环状 RNA(circRNAs)是一类非编码 RNA(ncRNAs),通过与 miRNA 结合可能调节基因表达。此外,最近的研究表明 circRNAs 参与了一些病理过程。然而,circDOCK1 在骨肉瘤(OS)中的表达及其生物学功能的知识仍存在很大空白。

方法

通过 circRNA 微阵列分析和定量实时 PCR(qRT-PCR)鉴定 OS 细胞系和组织中差异表达的 circRNAs。为了研究 circDOCK1 在体内和体外的作用,敲低或过表达 circDOCK1。为了评估 miR-339-3p、circDOCK1 和 IGF1R 之间的结合和调节关联,我们进行了挽救实验、RNA 免疫沉淀(RIP)、RNA 下拉测定和双荧光素酶测定。此外,我们进行了凋亡测定,以揭示 circDOCK1/miR-339-3p/IGF1R 轴对顺铂敏感性的调节作用。

结果

circDOCK1 在细胞质中的表达保持稳定,在 OS 组织和细胞中的表达高于相应对照。circDOCK1 的过表达增加了体内的致癌性和体外的恶性转化。在 U2OS 和 MG63 细胞系中,circDOCK1 通过海绵吸附 miR-339-3p 调节 IGF1R,从而调节肿瘤进展。此外,在 U2OS/DDP 和 MG63/DDP 细胞系中,circDOCK1 通过 miR-339-3p/IGF1R 轴调节顺铂敏感性。

结论

circDOCK1 通过 miR-339-3p/IGF1R 轴促进 OS 的进展并调节顺铂敏感性。因此,circDOCK1/miR-339-3p/IGF1R 轴可能是 OS 的关键机制和治疗靶点。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/fad9/8650521/476df1fc2f9c/12943_2021_1453_Fig1_HTML.jpg

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