假手术和神经损伤大鼠口腔面神经病变性疼痛临床前模型中转运蛋白- 18kd [TSPO]的正电子发射断层成像证明神经胶质反应性。

Q2 Medicine

Neurobiology of Pain Pub Date : 2025-01-01 DOI:10.1016/j.ynpai.2024.100175

Gaelle M. Emvalomenos , James W.M. Kang , Sabrina Salberg , Crystal Li , Bianca Jupp , Matthew Long , Mohammad B. Haskali , Sunil Kellapatha , OIivia I. Davanzo , Hyunsol Lim , Richelle Mychasiuk , Kevin A. Keay , Luke A. Henderson

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引用次数: 0

摘要

慢性神经性疼痛是由神经系统损伤引起的一种使人衰弱的疾病。目前的治疗在很大程度上是无效的，对潜在机制的了解有限，阻碍了有效治疗的发展。神经性疼痛的临床前模型显示，非神经变化对神经性疼痛的发展很重要，尽管这些数据几乎完全来自死后的组织学分析。尽管这些静态快照提供了有价值的数据，但它们不能提供非神经细胞变化的见解，而非神经细胞变化也可以在人类慢性疼痛患者中进行评估。在这项研究中，我们使用转运蛋白18 kDa (TSPO) PET成像与[18F]PBR06来观察三叉神经性疼痛啮齿动物临床前模型中巨噬细胞和小胶质细胞的活体活性。利用慢性眶下神经收缩损伤（ION-CCI），我们比较了雄性大鼠在ION-CCI之前和之后28天TSPO结合的时间变化，与假损伤和naïve对照相比。出乎意料的是，我们发现在手术和/或神经损伤后的初始阶段，离子- cci和假损伤大鼠三叉神经节、三叉神经脊髓核和叉旁核内的TSPO信号显著增加。这种增加的TSPO结合在第28天恢复到对照水平。对离子- cci和假损伤大鼠巨噬细胞积累和神经胶质反应性的定性组织学评价表明，三叉神经节巨噬细胞积累和脑干三叉神经复合体小胶质反应性。这些发现表明，在神经性疼痛的临床前模型中，神经损伤和假损伤大鼠的周围神经和大脑的胶质细胞变化为转化为人类患者提供了平台。

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Evidence for glial reactivity using positron-emission tomography imaging of translocator Protein-18 kD [TSPO] in both sham and nerve-injured rats in a preclinical model of orofacial neuropathic pain

Chronic neuropathic pain is a debilitating condition that results from damage to the nervous system. Current treatments are largely ineffective, with limited understanding of the underlying mechanisms hindering development of effective treatments. Preclinical models of neuropathic pain have revealed that non-neural changes are important for the development of neuropathic pain, although these data are derived almost exclusively from post-mortem histological analyses. Although these static snapshots have provided valuable data, they cannot provide insights into non-neural cell changes that could be also assessed in human patients with chronic pain. In this study we used translocator protein 18 kDa (TSPO) PET imaging with [¹⁸F]PBR06 to visualise in-vivo, the activity of macrophages and microglia in a rodent preclinical model of trigeminal neuropathic pain. Using chronic constriction injury of the infraorbital nerve (ION-CCI) we compared temporal changes in TSPO binding in male rats, prior to, and up to 28 days after ION-CCI compared with both sham-injured and naïve counterparts. Unexpectedly, we found significant increases in TSPO signal in both ION-CCI and sham-injured rats within the trigeminal ganglion, spinal trigeminal nucleus and paratrigeminal nucleus during the initial phase following surgery and/or nerve injury. This increased TSPO binding returned to control levels by day 28. Qualitative histological appraisal of macrophage accumulation and glial reactivity in both ION-CCI and sham-injured rats indicated macrophage accumulation in the trigeminal ganglion and microglial reactivity in the brainstem trigeminal complex. These findings show, glial changes in the peripheral nerve and brain in both nerve-injured and sham-injured rats in a preclinical model of neuropathic pain which provides a platform for translation into human patients.

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来源期刊

Neurobiology of Pain Medicine-Anesthesiology and Pain Medicine

CiteScore

4.40

自引率

0.00%

发文量

审稿时长

54 days