Urinary kallikrein reverses neuropathic pain by inhibiting ectopic neural discharges, neural inflammation and oxidative stress.

IF 2.2 4区 医学 Q3 TOXICOLOGY
Toxicology Research Pub Date : 2024-09-23 eCollection Date: 2024-10-01 DOI:10.1093/toxres/tfae146
Mingsheng Chen, Jinze Wu, Yafei Gao, Yunlei Li, Shiming He, Jungong Jin
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Abstract

Background: Neuropathic pain is a refractory disease and badly impacts the lives of patients. Urinary kallikrein (UK) acted as a glycoprotein has been discovered to play a pivotal role in neuroprotection. However, the regulatory impacts and correlative pathways of UK in the progression of neuropathic pain remain dimness.

Methods: The chronic constriction injury (CCI) rat model was firstly established to mimic neuropathic pain. The withdrawal threshold was measured through the Von Frey test. The levels of TNF-α, IL-1β and IL-6 were determined through ELISA. The levels of ROS, GSH, SOD and GSH-Px were examined through the commercial kits. The ectopic discharges were assessed. The protein expressions were inspected through western blot.

Results: It was demonstrated that withdrawal threshold was reduced in CCI rat model, but this change was reversed after UK treatment, indicating that UK relieved mechanical allodynia. Moreover, UK alleviated the inflammatory response through reducing TNF-α, IL-1β and IL-6 levels. It was uncovered that oxidative stress was strengthened in CCI rat model, but this impact was restrained after UK treatment. Additionally, UK suppressed ectopic discharge. At last, it was proved that UK triggered the Nrf2/ARE signaling pathway in CCI rat model.

Conclusion: This study manifested that UK reversed neuropathic pain by inhibiting ectopic neural pathways, neural pathways and oxidation via the Nrf2/ARE pathway. This study may offer useful proofs the regulatory functions of UK in the cure of neuropathic pain.

尿胆原通过抑制异位神经放电、神经炎症和氧化应激逆转神经病理性疼痛。
背景:神经病理性疼痛是一种难治性疾病,严重影响患者的生活。尿激酶(UK)作为一种糖蛋白被发现在神经保护中起着关键作用。然而,UK 在神经病理性疼痛进展过程中的调控影响和相关途径仍很模糊:方法:首先建立慢性收缩性损伤(CCI)大鼠模型来模拟神经病理性疼痛。方法:首先建立慢性收缩性损伤(CCI)大鼠模型,模拟神经病理性疼痛。通过酶联免疫吸附法测定 TNF-α、IL-1β 和 IL-6 的水平。通过商业试剂盒检测 ROS、GSH、SOD 和 GSH-Px 的水平。评估异位放电。通过 Western 印迹检测蛋白质表达:结果表明:CCI 大鼠模型的戒断阈值降低,但经过英国治疗后这一变化被逆转,表明英国缓解了机械异感。此外,UK 还能通过降低 TNF-α、IL-1β 和 IL-6 水平减轻炎症反应。研究发现,氧化应激在 CCI 大鼠模型中得到加强,但这种影响在 UK 治疗后得到抑制。此外,UK 还能抑制异位放电。最后,研究证明,UK 在 CCI 大鼠模型中触发了 Nrf2/ARE 信号通路:本研究表明,UK 可通过 Nrf2/ARE 通路抑制异位神经通路、神经通路和氧化,从而逆转神经病理性疼痛。本研究可为英国在治疗神经病理性疼痛方面的调节功能提供有益证明。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Toxicology Research
Toxicology Research TOXICOLOGY-
CiteScore
3.60
自引率
0.00%
发文量
82
期刊介绍: A multi-disciplinary journal covering the best research in both fundamental and applied aspects of toxicology
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