首页> 外文期刊>Journal of Endodontics: Official Journal of American Association of Endodontists >Direct effect of endodontic sealers on trigeminal neuronal activity
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Direct effect of endodontic sealers on trigeminal neuronal activity

机译:牙髓封闭剂对三叉神经元活动的直接作用

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Introduction Endodontic sealers are selected on the basis of their antimicrobial properties and ability to provide a tight seal. Sealer extrusions, whether intentional or unintentional, are common during obturation procedures. Such events have been correlated with increased postoperative discomfort and persistent pain states. However, the mechanisms underlying this phenomenon are largely unknown. Thus, we sought to evaluate the effect of commonly used endodontic sealers on peripheral nociceptors. We hypothesized that endodontic sealers can directly activate trigeminal nociceptors in a concentration- dependent manner, resulting in release of calcitonin gene-related peptide (CGRP), a potent modulator of neurogenic inflammation. Methods Rat trigeminal sensory neurons were exposed in vitro to vehicle, zinc oxide-eugenol (ZOE)-based sealer, AH Plus, EndoSequence BC sealer, or RealSeal SE. Neuronal activation was measured by quantification of neuropeptide (CGRP) release. In addition, cultured neurons were also subjected to the set form of all 4 sealers. The concentration of CGRP released was quantified by using a radioimmunoassay. Data were analyzed by using one-way analysis of variance with Newman-Keuls multiple comparison post hoc test. Results Both ZOE-based sealer and AH Plus in their fresh form evoked greater CGRP release than the control groups. Conversely, EndoSequence BC and RealSeal sealers both reduced basal GCRP release at all concentrations tested. Evaluation of the set sealers revealed that only ZOE-based sealer evoked significant CGRP release compared with its control group. Conclusions Overall, our results suggest that sealers can directly activate trigeminal nociceptors, leading to a robust release of CGRP, and may therefore lead to pain and neurogenic inflammation. This direct activation along with the immunologic response may underlie the symptoms and flare-up occurrences often seen with sealer extrusions.
机译:简介根管封闭剂的选择基于其抗菌性能和提供紧密密封的能力。封闭过程中,无论是有意还是无意的封口机挤压都很常见。此类事件与术后不适增加和持续性疼痛状态相关。但是,这种现象的潜在机制在很大程度上尚不清楚。因此,我们试图评估常用的牙髓封闭剂对周围伤害感受器的作用。我们假设,牙髓封闭剂可以浓度依赖的方式直接激活三叉神经痛感受器,从而导致降钙素基因相关肽(CGRP)的释放,这是神经源性炎症的有效调节剂。方法将大鼠三叉神经感觉神经元体外暴露于媒介物,基于氧化锌丁香酚(ZOE)的封闭剂,AH Plus,EndoSequence BC封闭剂或RealSeal SE。通过定量神经肽(CGRP)释放来测量神经元激活。此外,培养的神经元也要接受所有4种封闭剂的固定形式。通过放射免疫测定法定量释放的CGRP浓度。通过使用Newman-Keuls多重比较事后检验进行方差单向分析来分析数据。结果基于ZOE的封闭剂和新鲜形式的AH Plus均比对照组引起更大的CGRP释放。相反,EndoSequence BC和RealSeal封闭剂在所有测试浓度下均降低了基础GCRP释放。对固定密封剂的评估表明,与对照组相比,仅基于ZOE的密封剂可引起CGRP大量释放。结论总体而言,我们的结果表明,封闭剂可以直接激活三叉神经痛感受器,导致CGRP释放牢固,因此可能导致疼痛和神经源性炎症。这种直接激活以及免疫反应可能是密封剂挤压经常出现的症状和爆发现象的基础。

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