Miriam Santos-Caballero , Makeya A. Hasoun , Miguel Á. Huerta , M. Carmen Ruiz-Cantero , Miguel Á. Tejada , María Robles-Funes , Eduardo Fernández-Segura , Francisco J. Cañizares , Rafael González-Cano , Enrique J. Cobos
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Administered together, the compounds induced synergistic effects in the three aspects of postoperative pain, mirroring the known advantages of multimodal analgesia used in clinical practice. We explored the impact of neuroimmune interactions using a neutrophil depletion strategy. This reversed pain at rest and movement-induced pain, but did not alter cutaneous sensitivity. Non-peptidergic (IB4+) and peptidergic (CGRP+) nociceptors are segregated neuronal populations in the mouse. We tested the effects of gefapixant, an antitussive drug targeting non-peptidergic nociceptors through P2X3 antagonism, and olcegepant, an antimigraine drug acting as a CGRP antagonist. Both compounds reversed tactile allodynia, while only gefapixant reversed pain at rest, and none of them reversed movement-induced pain. In conclusion, tactile allodynia, pain at rest, and movement-induced pain after surgery have different pharmacological profiles, and none of the three aspects of postoperative pain can predict the effects of a given intervention on the other two. Combining these measures provides a more realistic view of postoperative pain and has the potential to benefit analgesic development.</p></div>","PeriodicalId":8966,"journal":{"name":"Biomedicine & Pharmacotherapy","volume":null,"pages":null},"PeriodicalIF":6.9000,"publicationDate":"2024-09-20","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"https://www.sciencedirect.com/science/article/pii/S0753332224013453/pdfft?md5=2e62cefbea02eddb86a2d756c4c7387d&pid=1-s2.0-S0753332224013453-main.pdf","citationCount":"0","resultStr":"{\"title\":\"Pharmacological differences in postoperative cutaneous sensitivity, pain at rest, and movement-induced pain in laparotomized mice\",\"authors\":\"Miriam Santos-Caballero , Makeya A. Hasoun , Miguel Á. Huerta , M. Carmen Ruiz-Cantero , Miguel Á. Tejada , María Robles-Funes , Eduardo Fernández-Segura , Francisco J. Cañizares , Rafael González-Cano , Enrique J. 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引用次数: 0
摘要
术后疼痛管理具有挑战性。我们利用小鼠的横向腹腔切口,研究了通过 von Frey 试验测量的触觉过敏、通过人工智能算法检测到的面部疼痛表情测量的静息痛,以及通过探索活动减少测量的运动诱发痛。吗啡和布洛芬这两种标准镇痛药产生了不同的结果依赖效应。与触觉过敏相比,吗啡能更有效地逆转静息时的疼痛,但却无法改变运动引起的疼痛。布洛芬在三种结果中的效果相当。同时使用这两种化合物会对术后疼痛的三个方面产生协同效应,这与临床实践中使用的多模式镇痛的已知优势相吻合。我们采用中性粒细胞耗竭策略探索了神经免疫相互作用的影响。这种方法逆转了静息时的疼痛和运动引起的疼痛,但没有改变皮肤的敏感性。小鼠的非肽能神经元(IB4+)和肽能神经元(CGRP+)痛觉感受器是分离的神经元群。我们测试了gefapixant(一种通过P2X3拮抗作用靶向非肽能性痛觉感受器的止咳药)和olcegepant(一种作为CGRP拮抗剂的抗偏头痛药)的作用。这两种化合物都能逆转触觉异感症,而只有吉非潘特能逆转静止时的疼痛,它们都不能逆转运动引起的疼痛。总之,术后触觉过敏、静息时疼痛和运动引起的疼痛具有不同的药理特征,术后疼痛的三个方面都无法预测特定干预对其他两个方面的影响。将这些测量方法结合起来可以更真实地反映术后疼痛的情况,并有可能有利于镇痛药的开发。
Pharmacological differences in postoperative cutaneous sensitivity, pain at rest, and movement-induced pain in laparotomized mice
Postoperative pain management is challenging. We used mice with a transverse laparotomy to study tactile allodynia measured by the von Frey test, pain at rest measured by facial pain expressions detected by an artificial intelligence algorithm, and movement-induced pain measured by reductions in exploratory activity. The standard analgesics morphine and ibuprofen induced distinct patterns of outcome-dependent effects. Whereas morphine was more effective in reversing pain at rest compared to tactile allodynia, it was unable to alter movement-induced pain. Ibuprofen showed comparable effects across the three outcomes. Administered together, the compounds induced synergistic effects in the three aspects of postoperative pain, mirroring the known advantages of multimodal analgesia used in clinical practice. We explored the impact of neuroimmune interactions using a neutrophil depletion strategy. This reversed pain at rest and movement-induced pain, but did not alter cutaneous sensitivity. Non-peptidergic (IB4+) and peptidergic (CGRP+) nociceptors are segregated neuronal populations in the mouse. We tested the effects of gefapixant, an antitussive drug targeting non-peptidergic nociceptors through P2X3 antagonism, and olcegepant, an antimigraine drug acting as a CGRP antagonist. Both compounds reversed tactile allodynia, while only gefapixant reversed pain at rest, and none of them reversed movement-induced pain. In conclusion, tactile allodynia, pain at rest, and movement-induced pain after surgery have different pharmacological profiles, and none of the three aspects of postoperative pain can predict the effects of a given intervention on the other two. Combining these measures provides a more realistic view of postoperative pain and has the potential to benefit analgesic development.
期刊介绍:
Biomedicine & Pharmacotherapy stands as a multidisciplinary journal, presenting a spectrum of original research reports, reviews, and communications in the realms of clinical and basic medicine, as well as pharmacology. The journal spans various fields, including Cancer, Nutriceutics, Neurodegenerative, Cardiac, and Infectious Diseases.