阿片类药物改变了行走时脚爪的位置,混淆了小鼠术后疼痛模型中镇痛效果的评估。

IF 3.4 Q2 NEUROSCIENCES
Pain Reports Pub Date : 2022-08-25 eCollection Date: 2022-09-01 DOI:10.1097/PR9.0000000000001035
Victoria E Brings, Maria A Payne, Robert W Gereau
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引用次数: 2

摘要

后爪定向实验是研究阿片类药物对小鼠镇痛作用的常用方法。然而,阿片类药物引起的过度运动可能会模糊这些检测的结果。目的:我们旨在通过步态分析来观察小鼠在行走过程中后爪的使用情况,以克服这种潜在的混淆。方法:观察术后疼痛诱导(采用爪切口模型)和羟考酮治疗后爪印面积的变化。结果:由于小鼠避免将后爪切开部分放置在地板上,故前爪切开手术减少了受伤后爪的爪印面积。令人惊讶的是,羟考酮使老鼠的步态像脚尖一样,减少了两只后爪的爪印面积。对这种阿片类药物诱导的表型的进一步研究表明,镇痛剂量的羟考酮或吗啡剂量依赖性地减少了未受伤小鼠的后爪印面积。步态变化不依赖于阿片类药物引起的运动活动的增加;在阿片类药物治疗的小鼠中,速度和爪印区域没有相关性,其他改变运动活动的镇痛化合物不影响爪印区域。结论:不幸的是,阿片类药物诱导的“脚尖”步态表型阻止了步态分析成为证明阿片类药物镇痛的可行指标。然而,这项工作揭示了一个重要的,以前未被描述的阿片类药物镇痛剂量对脚爪放置的影响。我们对阿片类药物如何影响步态的描述对使用小鼠研究阿片类药物药理学具有重要意义,并建议科学家在使用后爪导向的伤害性试验来测试小鼠阿片类药物镇痛时应谨慎。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Opioids alter paw placement during walking, confounding assessment of analgesic efficacy in a postsurgical pain model in mice.

Opioids alter paw placement during walking, confounding assessment of analgesic efficacy in a postsurgical pain model in mice.

Opioids alter paw placement during walking, confounding assessment of analgesic efficacy in a postsurgical pain model in mice.

Opioids alter paw placement during walking, confounding assessment of analgesic efficacy in a postsurgical pain model in mice.

Introduction: Hind paw-directed assays are commonly used to study the analgesic effects of opioids in mice. However, opioid-induced hyperlocomotion can obscure results of such assays.

Objectives: We aimed to overcome this potential confound by using gait analysis to observe hind paw usage during walking in mice.

Methods: We measured changes in the paw print area after induction of postsurgical pain (using the paw incision model) and treatment with oxycodone.

Results: Paw incision surgery reduced the paw print area of the injured hind paw as mice avoided placing the incised section of the paw on the floor. Surprisingly, oxycodone caused a tiptoe-like gait in mice, reducing the paw print area of both hind paws. Further investigation of this opioid-induced phenotype revealed that analgesic doses of oxycodone or morphine dose-dependently reduced the hind paw print area in uninjured mice. The gait changes were not dependent on opioid-induced increases in the locomotor activity; speed and paw print area had no correlation in opioid-treated mice, and other analgesic compounds that alter locomotor activity did not affect the paw print area.

Conclusion: Unfortunately, the opioid-induced "tiptoe" gait phenotype prevented gait analysis from being a viable metric for demonstrating opioid analgesia in injured mice. However, this work reveals an important, previously uncharacterized effect of treatment with analgesic doses of opioids on paw placement. Our characterization of how opioids affect gait has important implications for the use of mice to study opioid pharmacology and suggests that scientists should use caution when using hind paw-directed nociceptive assays to test opioid analgesia in mice.

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来源期刊
Pain Reports
Pain Reports Medicine-Anesthesiology and Pain Medicine
CiteScore
7.50
自引率
2.10%
发文量
93
审稿时长
8 weeks
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