急性颈肌炎症后,上颈段浅层背角神经元突触和内在特性的对比变化。
Contrasting alterations to synaptic and intrinsic properties in upper-cervical superficial dorsal horn neurons following acute neck muscle inflammation.
机构信息
School of Biomedical Sciences and Pharmacy, Faculty of Health and Medicine, The University of Newcastle and Hunter Medical Research Institute, Room 411 Medical Sciences Building, University Drive, Newcastle, NSW 2308, Australia.
出版信息
Mol Pain. 2014 Apr 12;10:25. doi: 10.1186/1744-8069-10-25.
BACKGROUND
Acute and chronic pain in axial structures, like the back and neck, are difficult to treat, and have incidence as high as 15%. Surprisingly, most preclinical work on pain mechanisms focuses on cutaneous structures in the limbs and animal models of axial pain are not widely available. Accordingly, we developed a mouse model of acute cervical muscle inflammation and assessed the functional properties of superficial dorsal horn (SDH) neurons.
RESULTS
Male C57/Bl6 mice (P24-P40) were deeply anaesthetised (urethane 2.2 g/kg i.p) and the rectus capitis major muscle (RCM) injected with 40 μl of 2% carrageenan. Sham animals received vehicle injection and controls remained anaesthetised for 2 hrs. Mice in each group were sacrificed at 2 hrs for analysis. c-Fos staining was used to determine the location of activated neurons. c-Fos labelling in carrageenan-injected mice was concentrated within ipsilateral (87% and 63% of labelled neurons in C1 and C2 segments, respectively) and contralateral laminae I - II with some expression in lateral lamina V. c-Fos expression remained below detectable levels in control and sham animals. In additional experiments, whole cell recordings were obtained from visualised SDH neurons in transverse slices in the ipsilateral C1 and C2 spinal segments. Resting membrane potential and input resistance were not altered. Mean spontaneous EPSC amplitude was reduced by ~20% in neurons from carrageenan-injected mice versus control and sham animals (20.63 ± 1.05 vs. 24.64 ± 0.91 and 25.87 ± 1.32 pA, respectively). The amplitude (238 ± 33 vs. 494 ± 96 and 593 ± 167 pA) and inactivation time constant (12.9 ± 1.5 vs. 22.1 ± 3.6 and 15.3 ± 1.4 ms) of the rapid A type potassium current (IAr), the dominant subthreshold current in SDH neurons, were reduced in carrageenan-injected mice.
CONCLUSIONS
Excitatory synaptic drive onto, and important intrinsic properties (i.e., IAr) within SDH neurons are reduced two hours after acute muscle inflammation. We propose this time point represents an important transition period between peripheral and central sensitisation with reduced excitatory drive providing an initial neuroprotective mechanism during the early stages of the progression towards central sensitisation.
背景
轴向结构(如背部和颈部)的急性和慢性疼痛难以治疗,发病率高达 15%。令人惊讶的是,大多数关于疼痛机制的临床前工作都集中在四肢的皮肤结构上,并且轴向疼痛的动物模型并不广泛可用。因此,我们开发了一种急性颈肌炎症的小鼠模型,并评估了浅层背角(SDH)神经元的功能特性。
结果
雄性 C57/Bl6 小鼠(P24-P40)被深度麻醉(腹腔内给予 2.2 g/kg 尿嘧啶),并向头长肌(RCM)注射 40 μl 2%角叉菜胶。假手术动物接受载体注射,对照组麻醉 2 小时。每组动物在 2 小时时处死进行分析。使用 c-Fos 染色来确定激活神经元的位置。角叉菜胶注射小鼠的 c-Fos 标记集中在同侧(C1 和 C2 节段的 87%和 63%的标记神经元)和对侧 I-II 层,在外侧 V 层有一些表达。在对照和假手术动物中,c-Fos 表达仍低于可检测水平。在额外的实验中,从同侧 C1 和 C2 脊髓段的横切片中获得了可视化 SDH 神经元的全细胞膜片钳记录。静息膜电位和输入电阻没有改变。与对照和假手术动物相比,来自角叉菜胶注射小鼠的神经元的平均自发 EPSC 幅度降低了约 20%(20.63±1.05 对 24.64±0.91 和 25.87±1.32 pA)。快速 A 型钾电流(IAr)的幅度(238±33 对 494±96 和 593±167 pA)和失活时间常数(12.9±1.5 对 22.1±3.6 和 15.3±1.4 ms)在角叉菜胶注射小鼠中降低。
结论
急性肌肉炎症后 2 小时,SDH 神经元上的兴奋性突触传入和重要的内在特性(即 IAr)降低。我们提出,这一时间点代表外周和中枢敏化之间的重要过渡阶段,兴奋性驱动的降低为中枢敏化进展的早期阶段提供了初始的神经保护机制。
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