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首页> 外文期刊>Journal of clinical laboratory analysis. >The role of circRNA derived from RUNX2 in the serum of osteoarthritis and its clinical value
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The role of circRNA derived from RUNX2 in the serum of osteoarthritis and its clinical value

机译:Circrna衍生自Runx2在骨关节炎血清中的作用及其临床价值

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摘要

Background Circular RNA (circRNA) has been shown to affect the pathological process of osteoarthritis (OA) and is expected to become a potential marker for disease diagnosis. This study aimed to investigate the association between circRNA derived from the gene of runt-related transcription factor 2 (RUNX2) and OA risk. Methods The expression profile of RUNX2-derived circRNAs in serum of OA patients was detected. Then, the cytological localization of screened differential circRNAs was studied. Luciferase (LUC) reporter assay was used to identify the microRNA (miRNA) sponge capacity of the circRNAs. Bioinformatics analysis was used to construct the functional pathway of this circRNA-miRNAs network. And then, the diagnostic value of RUNX2-derived circRNAs in OA was evaluated. Results RUNX2-derived hsa_circ_0005526 (circ_RUNX2) is significantly highly expressed in OA serum and mainly located in the cytoplasm within the cartilage cell by sponging multiple miRNAs (miR-498, miR-924, miR-361-3p, and miR-665). Bioinformatics analysis showed ECM-receptor interaction pathway ranked the most significant pathway of circ_RUNX2-miRNAs regulatory network in KEGG database. The ROC curve showed that there may be good diagnostic value of serum circ_RUNX2 in OA. Conclusion RUNX2-derived circ_RUNX2 may be involved in OA development via ECM-receptor interaction pathways and may be used as potential clinical indicator of OA.
机译:背景技术已被证明圆形RNA(CircrNA)影响骨关节炎(OA)的病理过程,并且预计将成为疾病诊断的潜在标志物。该研究旨在探讨来自runt相关转录因子2(Runx2)和OA风险的源自源自衍生的CircrNA之间的关联。方法检测OA患者血清中runx2衍生rERCRNA的表达谱。然后,研究了筛选的差分晶圆的细胞学定位。荧光素酶(LUC)报告分析用于鉴定Circrnas的microRNA(miRNA)海绵容量。生物信息学分析用于构建该CircRNA-MiRNA网络的功能途径。然后,评估OA中的Runx2派生Circrnas的诊断值。结果在OA血清中显着高度表达Runx2-ermirc_0005526(Circ_runx2),主要在软骨细胞内的细胞质中,通过海绵到多个miRNA(miR-498,miR-924,miR-361-3p和miR-665)。生物信息学分析显示ECM受体相互作用途径在Kegg数据库中排名Circ_Runx2-MiRNAS监管网络中最显着的途径。 ROC曲线表明,OA中可能存在血清Circ_runx2的良好诊断值。结论RUNX2衍生的CIRC_RUNX2可以通过ECM-受体相互作用途径参与OA显影,并且可以用作OA的潜在临床指标。

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