探索异鼠李素的镇痛潜力:福尔马林诱导疼痛和糖尿病神经病变模型的启示。

IF 3.3 4区 医学 Q1 Medicine
A Alqudah, E Qnais, Y Bseiso, O Gammoh, M Wedyan, M Oqal, R AbuDalo, B S Alotaibi
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引用次数: 0

摘要

目的:异鼠李素是一种天然黄酮类化合物,是多种药用植物的主要成分,具有极其重要的药理作用。本研究旨在通过福尔马林诱导的疼痛和糖尿病神经病变情景,研究异鼠李素在小鼠模型中的镇痛特性:为了实现我们的目标,给小鼠口服不同剂量(10 至 100 毫克/千克)的异鼠李素。在第二阶段使用福尔马林试验评估与疼痛相关的行为。此外,我们还在链脲佐菌素诱导的糖尿病神经病变模型中评估了异鼠李素的潜在镇痛效果。此外,我们还在福尔马林试验中使用了纳洛酮(众所周知的阿片受体拮抗剂)、育亨宾(阻断α2-肾上腺素能受体)和甲氰菊酯(抑制血清素能受体)等高级干预药物:结果:在福尔马林诱导的福尔马林试验第二阶段,口服异鼠李素可减少与疼痛相关的行为,减少的程度与观察到的剂量成正比。在糖尿病神经病变模型中,服用异鼠李素可有效逆转所观察到的疼痛阈值降低。值得注意的是,在福尔马林试验中,阿片受体拮抗剂纳洛酮能有效抵消异鼠李素产生的镇痛效果,而育亨宾和甲塞酮则没有产生类似的效果。异鼠李素还能降低福尔马林引发的脊髓环磷酸腺苷(cAMP)反应元件结合蛋白(CREB)水平的升高,而预纳洛酮处理则可逆转这种效应。该化合物还能抑制糖尿病神经病变引起的脊髓磷酸化 CREB(p-CREB)水平升高:本研究确定,异鼠李素在福尔马林诱导的疼痛和糖尿病神经病变模型中具有显著的镇痛能力。在福尔马林诱导的疼痛模型中,异鼠李素的止痛机制似乎与激活脊髓阿片受体和调整 CREB 蛋白数量有关。这一发现使我们进一步了解了如何利用异鼠李素治疗福尔马林诱导的疼痛和糖尿病神经病变引起的疼痛。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Exploring the analgesic potential of isorhamnetin: insights from formalin-induced pain and diabetic neuropathy models.

Objective: Isorhamnetin, a naturally occurring flavonoid compound, holds paramount importance as a primary constituent within several medicinal plants, exhibiting profound pharmacological significance. The aim of this study is to investigate the pain-relieving attributes of isorhamnetin in murine models through both formalin-induced pain and diabetic neuropathy scenarios.

Materials and methods: To achieve our objective, isorhamnetin was orally administered to mice at varying dosage levels (10 to 100 mg/kg). Pain-related behaviors were assessed using the formalin test during its secondary phase. Additionally, the potential pain-alleviating effect of isorhamnetin was evaluated in a diabetic neuropathy model induced by streptozotocin. Additionally, we carried out advanced interventions using naloxone, which is a well-known antagonist of opioid receptors, yohimbine, which blocks α2-adrenergic receptors, and methysergide, which inhibits serotonergic receptors, during the formalin test.

Results: The oral intake of isorhamnetin showed a decrease in behaviors associated with pain that was proportional to the dose observed during the second phase of the formalin test when induced by formalin. In the diabetic neuropathy model, isorhamnetin administration effectively reversed the reduced pain threshold observed. Notably, naloxone, the opioid receptor antagonist, effectively counteracted the pain-relieving effect produced by isorhamnetin in the formalin test, whereas yohimbine and methysergide did not yield similar outcomes. Isorhamnetin also led to a reduction in elevated spinal cyclic adenosine monophosphate (cAMP) response element binding protein (CREB) levels triggered by formalin, with this effect reversed by pre-treatment with naloxone. The compound also suppressed heightened spinal phosphorylated CREB (p-CREB) levels caused by diabetic neuropathy.

Conclusions: This research determined that isorhamnetin has notable abilities to relieve pain in models of formalin-induced pain and diabetic neuropathy. The pain-relieving mechanism of isorhamnetin in the formalin-induced pain model seems to be connected to the activation of spinal opioid receptors and the adjustment of CREB protein amounts. This insight improves our knowledge of how isorhamnetin could be used therapeutically to treat pain conditions stemming from formalin-induced pain and diabetic neuropathy.

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来源期刊
CiteScore
5.30
自引率
6.10%
发文量
906
审稿时长
2-4 weeks
期刊介绍: European Review for Medical and Pharmacological Sciences, a fortnightly journal, acts as an information exchange tool on several aspects of medical and pharmacological sciences. It publishes reviews, original articles, and results from original research. The purposes of the Journal are to encourage interdisciplinary discussions and to contribute to the advancement of medicine. European Review for Medical and Pharmacological Sciences includes: -Editorials- Reviews- Original articles- Trials- Brief communications- Case reports (only if of particular interest and accompanied by a short review)
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