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首页> 外文期刊>Arthritis research & therapy. >Up-regulation of circulating microRNA-17 is associated with lumbar radicular pain following disc herniation
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Up-regulation of circulating microRNA-17 is associated with lumbar radicular pain following disc herniation

机译:椎间盘突出症后循环microRNA-17的上调与腰根​​根痛有关

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摘要

Previous studies suggest that regulatory microRNAs (miRs) may modulate neuro-inflammatory processes. The purpose of the present study was to examine the role of miR-17 following intervertebral disc herniation. In a cohort of 97 patients with leg pain and disc herniation verified on MRI, we investigated the association between circulating miR-17 and leg pain intensity. A rat model was used to examine possible changes in miR-17 expression in nucleus pulposus (NP) associated with leak of NP tissue out of the herniated disc. The functional role of miR-17 was addressed by transfection of miR-17 into THP-1 cells (human monocyte cell line). An association between the level of miR-17 in serum and the intensity of lumbar radicular pain was shown. Up-regulation of miR-17 in the rat NP tissue when applied onto spinal nerve roots and increased release of TNF following transfection of miR-17 into THP-1 cells were also observed. Hence, our data suggest that miR-17 may be involved in the pathophysiology underlying lumbar radicular pain after disc herniation. We conclude that miR-17 may be associated with the intensity of lumbar radicular pain after disc herniation, possibly through a TNF-driven pro-inflammatory mechanism.
机译:先前的研究表明调节性microRNA(miRs)可能会调节神经炎症过程。本研究的目的是检查椎间盘突出后miR-17的作用。在MRI验证的97例腿部疼痛和椎间盘突出症患者中,我们调查了循环miR-​​17与腿部疼痛强度之间的关系。使用大鼠模型检查髓核(NP)中miR-17表达的可能变化,该变化与NP组织从椎间盘漏出有关。通过将miR-17转染入THP-1细胞(人单核细胞系)来解决miR-17的功能作用。血清中的miR-17水平与腰部神经根疼痛的强度之间存在关联。当将miR-17转染到THP-1细胞后,还观察到大鼠NP组织中miR-17的上调和TNF释放的增加。因此,我们的数据表明,miR-17可能参与了椎间盘突出症后腰神经根疼痛的病理生理。我们得出的结论是,miR-17可能与椎间盘突出症后腰神经根疼痛的强度有关,可能是通过TNF驱动的促炎机制引起的。

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