Long-term neuropathic pain behaviors correlate with synaptic plasticity and limbic circuit alteration: a comparative observational study in mice

SNi公司 神经病理性疼痛 前额叶皮质 神经损伤 神经科学 伏隔核 医学 海马体 齿状回 突触可塑性 周围神经损伤 长时程增强 边缘下皮质 神经可塑性 心理学 麻醉 中枢神经系统 认知 坐骨神经 内科学 生物 受体 生物化学 水解 酸水解
作者
Francesca Guida,Monica Iannotta,Gabriella Misso,Flavia Ricciardi,Serena Boccella,Virginia Tirino,Michela Falco,Vincenzo Desiderio,Rosmara Infantino,Gorizio Pieretti,Vito de Novellis,Gianpaolo Papaccio,Livio Luongo,Michele Caraglia,Sabatino Maione
出处
期刊:Pain [Lippincott Williams & Wilkins]
卷期号:163 (8): 1590-1602 被引量:4
标识
DOI:10.1097/j.pain.0000000000002549
摘要

Neuropathic pain has long-term consequences in affective and cognitive disturbances, suggesting the involvement of supraspinal mechanisms. In this study, we used the spared nerve injury (SNI) model to characterize the development of sensory and aversive components of neuropathic pain and to determine their electrophysiological impact across prefrontal cortex and limbic regions. Moreover, we evaluated the regulation of several genes involved in immune response and inflammation triggered by SNI. We showed that SNI led to sensorial hypersensitivity (cold and mechanical stimuli) and depressive-like behavior lasting 12 months after nerve injury. Of interest, changes in nonemotional cognitive tasks (novel object recognition and Y maze) showed in 1-month SNI mice were not evident normal in the 12-month SNI animals. In vivo electrophysiology revealed an impaired long-term potentiation at prefrontal cortex-nucleus accumbens core pathway in both the 1-month and 12-month SNI mice. On the other hand, a reduced neural activity was recorded in the lateral entorhinal cortex-dentate gyrus pathway in the 1-month SNI mice, but not in the 12-month SNI mice. Finally, we observed the upregulation of specific genes involved in immune response in the hippocampus of 1-month SNI mice, but not in the 12-month SNI mice, suggesting a neuroinflammatory response that may contribute to the SNI phenotype. These data suggest that distinct brain circuits may drive the psychiatric components of neuropathic pain and pave the way for better investigation of the long-term consequences of peripheral nerve injury for which most of the available drugs are to date unsatisfactory.

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