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鞘内长期暴露于γ干扰素后大鼠背角神经元在体内的反应性增强。

Increased responsiveness of rat dorsal horn neurons in vivo following prolonged intrathecal exposure to interferon-gamma.

作者信息

Vikman K S, Siddall P J, Duggan A W

机构信息

Pain Management Research Institute, University of Sydney at Royal North Shore Hospital, St. Leonards, NSW, 2065, Australia.

出版信息

Neuroscience. 2005;135(3):969-77. doi: 10.1016/j.neuroscience.2005.06.059. Epub 2005 Aug 26.

Abstract

Prolonged increases in the level of the pro-inflammatory cytokine interferon-gamma occur in the CNS during some disease states associated with persistent pain. Administration of interferon-gamma to both humans and rodents has produced pain or pain-related behavior but the underlying mechanisms are unknown. The present study examined the effects of repeated intrathecal administration of interferon-gamma on dorsal horn neuronal responses under in vivo conditions. In addition, behavioral effects of interferon-gamma treatment were studied. Intrathecal cannulae were implanted into anesthetized rats. Animals then received either 1000 U of recombinant rat interferon-gamma in 10 microl buffer intrathecally, repeated four times over 8 days, or similarly administered buffer (controls). Interferon-gamma-treated animals showed a significant reduction in paw withdrawal threshold to mechanical stimulation of the hind paw. Electrophysiological experiments were performed under halothane anesthesia. Extracellular recordings of spontaneous and evoked responses were obtained from dorsal horn neurons (n=64) in the lumbar spinal cord. There was a significantly higher proportion of spontaneously active neurons in the interferon-gamma-treated animals (50%) when compared with controls (19%). A significantly increased proportion of neurons from interferon-gamma-treated animals displayed afterdischarges following both innocuous and noxious mechanical stimulation of the receptive field (brush: 21% in interferon-gamma-treated, 3% in controls; pinch: 97% in interferon-gamma-treated, 50% in controls). Neurons from interferon-gamma-treated animals also showed significantly increased wind-up of action potentials in response to repeated electrical stimulation of the sciatic nerve at C-fiber strength at both 0.5 and 1 Hz. Paired-pulse inhibition, evoked through electrical stimulation of the cutaneous receptive field, was significantly decreased in neurons from interferon-gamma-treated animals at 50 and 100 ms inter-stimulus intervals. We propose that this demonstrated reduction in inhibition may underlie the enhanced excitatory responses. Such interferon-gamma-induced changes in evoked responses may contribute to persistent pain following damage or disease states in the nervous system.

摘要

在一些与持续性疼痛相关的疾病状态下,中枢神经系统中促炎细胞因子干扰素-γ水平会持续升高。给人类和啮齿动物注射干扰素-γ会产生疼痛或与疼痛相关的行为,但其潜在机制尚不清楚。本研究在体内条件下检测了重复鞘内注射干扰素-γ对背角神经元反应的影响。此外,还研究了干扰素-γ治疗的行为效应。将鞘内套管植入麻醉的大鼠体内。然后,动物接受鞘内注射10微升缓冲液中1000单位重组大鼠干扰素-γ,在8天内重复4次,或同样注射缓冲液(对照组)。接受干扰素-γ治疗的动物对后爪机械刺激的爪退缩阈值显著降低。在氟烷麻醉下进行电生理实验。从腰脊髓背角神经元(n = 64)获得自发和诱发反应的细胞外记录。与对照组(19%)相比,接受干扰素-γ治疗的动物中自发活动神经元的比例显著更高(50%)。接受干扰素-γ治疗的动物中,在对感受野进行无害和有害机械刺激后,出现后放电的神经元比例显著增加(轻刷:干扰素-γ治疗组为21%,对照组为3%;捏压:干扰素-γ治疗组为97%,对照组为50%)。接受干扰素-γ治疗的动物的神经元在0.5和1赫兹时,对坐骨神经以C纤维强度进行重复电刺激时,动作电位的累加也显著增加。通过对皮肤感受野进行电刺激诱发的配对脉冲抑制,在接受干扰素-γ治疗的动物的神经元中,在刺激间隔为50和100毫秒时显著降低。我们认为,这种已证明的抑制作用降低可能是兴奋性反应增强的基础。这种干扰素-γ诱导的诱发反应变化可能导致神经系统损伤或疾病状态后的持续性疼痛。

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