University of Texas at Dallas, School of Behavioral and Brain Sciences, Richardson, Texas 75080, and.
Departments of Neurobiology and Otolaryngology, Pittsburgh Center for Pain Research, University of Pittsburgh School of Medicine, Pittsburgh, Pennsylvania 16206.
J Neurosci. 2018 Jan 10;38(2):379-397. doi: 10.1523/JNEUROSCI.2110-17.2017. Epub 2017 Nov 22.
Dopaminergic modulation of spinal cord plasticity has long been recognized, but circuits affected by this system and the precise receptor subtypes involved in this modulation have not been defined. Dopaminergic modulation from the A11 nucleus of the hypothalamus contributes to plasticity in a model of chronic pain called hyperalgesic priming. Here we tested the hypothesis that the key receptor subtype mediating this effect is the D5 receptor (D5R). We find that a spinally directed lesion of dopaminergic neurons reverses hyperalgesic priming in both sexes and that a D1/D5 antagonist transiently inhibits neuropathic pain. We used mice lacking D5Rs ( mice) to show that carrageenan, interleukin 6, as well as BDNF-induced hyperalgesia and priming are reduced specifically in male mice. These male mice also show reduced formalin pain responses and decreased heat pain. To characterize the subtypes of dorsal horn neurons engaged by dopamine signaling in the hyperalgesic priming model, we used c-fos labeling. We find that a mixed D1/D5 agonist given spinally to primed mice activates a subset of neurons in lamina III and IV of the dorsal horn that coexpress PAX2, a transcription factor for GABAergic interneurons. In line with this, we show that gabazine, a GABA-A receptor antagonist, is antihyperalgesic in primed mice exposed to spinal administration of a D1/D5 agonist. Therefore, the D5R, in males, and the D1R, in females, exert a powerful influence over spinal cord circuitry in pathological pain likely via modulation of deep dorsal horn GABAergic neurons. Pain is the most prominent reason why people seek medical attention, and chronic pain incidence worldwide has been estimated to be as high as 33%. This study provides new insight into how descending dopamine controls pathological pain states. Our work demonstrates that dopaminergic spinal projections are necessary for the maintenance of a chronic pain state in both sexes; however, D5 receptors seem to play a critical role in males whereas females rely more heavily on D1 receptors, an effect that could be explained by sexual dimorphisms in receptor expression levels. Collectively, our work provides new insights into how the dopaminergic system interacts with spinal circuits to promote pain plasticity.
长期以来,人们一直认识到多巴胺能调制脊髓可塑性,但受该系统影响的回路以及参与这种调制的确切受体亚型尚未确定。下丘脑 A11 核的多巴胺能调制有助于一种称为痛觉过敏引发的慢性疼痛模型中的可塑性。在这里,我们测试了这样一个假设,即介导这种效应的关键受体亚型是 D5 受体 (D5R)。我们发现,多巴胺能神经元的脊髓定向损伤可逆转两性的痛觉过敏引发,并且 D1/D5 拮抗剂可短暂抑制神经病理性疼痛。我们使用缺乏 D5R 的小鼠 ( mice) 表明,角叉菜胶、白细胞介素 6 以及 BDNF 诱导的痛觉过敏和引发在雄性小鼠中特异性减少。这些雄性 mice 还表现出福尔马林疼痛反应减少和热痛觉降低。为了表征痛觉过敏引发模型中背角神经元中多巴胺信号参与的亚型,我们使用了 c-fos 标记。我们发现,给引发的小鼠脊髓内给予混合的 D1/D5 激动剂可激活背角 III 和 IV 层中表达 PAX2 的神经元亚群,PAX2 是 GABA 能中间神经元的转录因子。与此一致,我们表明,GABA-A 受体拮抗剂 gabazine 在接受脊髓内给予 D1/D5 激动剂的引发小鼠中具有抗痛觉过敏作用。因此,D5R 在雄性中,D1R 在雌性中,通过调制深部背角 GABA 能神经元,对病理性疼痛中的脊髓环路产生强大影响。疼痛是人们寻求医疗关注的最突出原因,全球慢性疼痛的发生率估计高达 33%。这项研究为下行多巴胺如何控制病理性疼痛状态提供了新的见解。我们的工作表明,多巴胺能脊髓投射对于维持两性的慢性疼痛状态是必要的;然而,D5 受体似乎在雄性中起着关键作用,而雌性则更依赖于 D1 受体,这种效应可以通过受体表达水平的性别二态性来解释。总之,我们的工作提供了新的见解,即多巴胺能系统如何与脊髓回路相互作用以促进疼痛可塑性。
