Reversal of neuropathic pain is associated with corticostriatal functional reorganization after nerve repair in the spared nerve injury model

神经病理性疼痛 痛觉超敏 SNi公司 神经损伤 医学 周围神经损伤 麻醉 神经再支配 痛觉过敏 伤害 神经痛 假手术 神经科学 坐骨神经 外科 内科学 心理学 病理 化学 生物化学 受体 替代医学 水解 酸水解
作者
Qiyuan Bao,Pei-Ching Chang,Maria Virginia Centeno,Melissa A. Farmer,Marwan N. Baliki,Daniel Procissi,Weibin Zhang,A. Vania Apkarian
出处
期刊:Pain [Lippincott Williams & Wilkins]
卷期号:163 (10): 1929-1938 被引量:3
标识
DOI:10.1097/j.pain.0000000000002590
摘要

Following surgical repair after peripheral nerve injury, neuropathic pain diminishes in most patients but can persist in a small proportion of cases, the mechanism of which remains poorly understood. Based on the spared nerve injury (SNI), we developed a rat nerve repair (NR) model, where a delayed reconstruction of the SNI-injured nerves resulted in alleviating chronic pain-like behavior only in a subpopulation of rats. Multiple behavioral measures were assayed over 11-week presurgery and postsurgery periods (tactile allodynia, pain prick responses, sucrose preference, motor coordination, and cold allodynia) in SNI (n = 10), sham (n = 8), and NR (n = 12) rats. All rats also underwent resting-state functional magnetic resonance imaging under anesthesia at multiple time points postsurgery, and at 10 weeks, histology and retrograde labeling were used to calculate peripheral reinnervation. Behavioral measures indicated that at approximately 5 weeks postsurgery, the NR group separated to pain persisting (NR persisting, n = 5) and recovering (NR recovering, n = 7) groups. Counts of afferent nerves and dorsal root ganglion cells were not different between NR groups. Therefore, NR group differences could not be explained by peripheral reorganization. By contrast, large brain functional connectivity differences were observed between NR groups, where corticolimbic reorganization paralleled with pain recovery (repeated-measures analysis of variance, false discovery rate, P < 0.05), and functional connectivity between accumbens and medial frontal cortex was related both to tactile allodynia (nociception) and to sucrose preference (anhedonia) in the NR group. Our study highlights the importance of brain circuitry in the reversal of neuropathic pain as a natural pain-relieving mechanism. Further studies regarding the therapeutic potentials of these processes are warranted.
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