首页> 外文期刊>Neuroscience Letters: An International Multidisciplinary Journal Devoted to the Rapid Publication of Basic Research in the Brain Sciences >Dopamine D3 receptor regulates basal but not amphetamine-induced changes in pain sensitivity in mice.
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Dopamine D3 receptor regulates basal but not amphetamine-induced changes in pain sensitivity in mice.

机译:多巴胺D3受体调节小鼠的痛觉敏感性中的基础而非苯丙胺诱导的变化。

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摘要

Pain is a complex and subjective experience that involves not only the transduction of noxious stimuli by nociceptive fibers, but also the cognitive and emotional processing by the brain. Previous studies on the transmission of nociception suggest that the activation of mesolimbic dopamine (DA) system plays an important role in mediating the suppression of tonic pain. The aim of the current study was to examine the role of DA D3 receptor in modulating basal and amphetamine-induced changes in pain sensitivity in mice. We used wild-type and D3 receptor mutant mice and determined allodynia induced by both noxious heat (radiant heat) and mechanical (von Frey hair) stimuli. We show that D3 receptor mutant mice exhibit hypoalgesia in both the tail-flick test and von Frey hair test compared to wild-type mice. Amphetamine-induced hyperalgesia in both D3 receptor mutant and wild-type mice in the tail-flick test and von Frey hair test. There was no significantly difference in the relative change in pain sensitivity between wild-type and D3 receptor mutant mice in both the tail-flick test and von Frey hair test following amphetamine administration. These results suggest that the D3 receptor regulates the transmission of nociception. Moreover, amphetamine can lower pain threshold in mice.
机译:疼痛是一种复杂而主观的经历,不仅涉及伤害感受纤维对有害刺激的转导,而且还涉及大脑的认知和情感加工。先前对伤害感受传递的研究表明,中脑边缘多巴胺(DA)系统的激活在调节镇痛方面起着重要作用。本研究的目的是研究DA D3受体在调节基础和苯丙胺诱导的小鼠疼痛敏感性变化中的作用。我们使用了野生型和D3受体突变小鼠,并确定了由有害热(辐射热)和机械刺激(冯·弗雷毛发)引起的异常性疼痛。我们显示,与野生型小鼠相比,D3受体突变型小鼠在甩尾试验和冯·弗雷毛发试验中均表现出痛觉过敏。在甩尾试验和冯·弗雷毛发试验中,D3受体突变体和野生型小鼠中苯丙胺引起的痛觉过敏。在安非他明给药后的甩尾试验和冯·弗雷毛发试验中,野生型和D3受体突变型小鼠的疼痛敏感性相对变化无明显差异。这些结果表明,D3受体调节伤害感受的传递。此外,苯丙胺可以降低小鼠的疼痛阈值。

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