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The Long Noncoding RNA MEG3 Is Downregulated and Inversely Associated with VEGF Levels in Osteoarthritis

机译:长度非编码RNA Meg3下调并与骨关节炎的VEGF水平反比

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摘要

Osteoarthritis (OA) is becoming a major public health problem in China, especially considering the increase in average life expectancy of the population. Thus, enhanced understanding of the molecular changes associated with OA is urgently needed to develop more effective strategies for the diagnosis and treatment of this debilitating disease. LncRNAs play an important role in the processes of bone and cartilage development. Maternally expressed gene 3 (MEG3) is a maternally expressed lncRNA and may function as a tumor suppressor by inhibiting angiogenesis. OA is closely associated with angiogenesis and the inhibition of angiogenesis presents a novel therapeutic approach to reduce inflammation and pain in OA. In this study, we detected the mRNA expression of MEG3 and VEGF in articular cartilage samples from 20 OA patients and 10 healthy volunteers by real-time RT-PCR. VEGF protein is detected by ELISA in cartilage samples. The results show that human MEG3 is significantly downregulated in OA patients compared to normal cartilage samples. However, higher levels of VEGF mRNA and protein are found in OA compared to the control. Moreover, MEG3 levels are inversely associated with VEGF levels, suggesting that MEG3 may be involved in OA development through the regulation of angiogenesis.
机译:骨关节炎(OA)正在成为中国的主要公共卫生问题,特别是考虑到人口平均预期寿命的增加。因此,迫切需要增强对与OA相关的分子变化的理解,以开发更有效的诊断和治疗这种衰弱疾病的策略。 LNCRNA在骨骼和软骨开发过程中发挥着重要作用。母体表达的基因3(MEG3)是母体表达的LNCRNA,可以通过抑制血管生成来用作肿瘤抑制剂。 OA与血管生成密切相关,血管生成的抑制呈现了一种新的治疗方法,以减少OA中的炎症和疼痛。在这项研究中,通过实时RT-PCR检测了来自20个患者和10名健康志愿者的关节软骨样品中MEG3和VEGF的mRNA表达。通过ELISA在软骨样品中检测到VEGF蛋白。结果表明,与正常软骨样品相比,人类MEG3在OA患者中显着下调。然而,与对照相比,OA中发现了更高水平的VEGF mRNA和蛋白质。此外,MEG3水平与VEGF水平反向相关,表明MEG3可以通过血管生成的调节涉及OA开发。

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