Zhang Z, Zhang Z-Y, Fauser U, Schluesener H J
Institute of Brain Research, University of Tuebingen, Tuebingen, Germany.
Neuroscience. 2008 Mar 18;152(2):495-501. doi: 10.1016/j.neuroscience.2007.12.042. Epub 2008 Jan 12.
Experimental autoimmune neuritis (EAN) is the animal model of acute inflammatory demyelinating polyradiculoneuropathy (AIDP) that is the most common subtype of Guillain-Barre syndrome (GBS). While neuropathic pain is a common symptom of GBS, its underlying mechanisms remain elusive. Central sensitization, particularly spinal glia (microglia and astrocytes) activation, is important for the initiation and maintenance of neuropathic pain. P2X(4) receptor (P2X(4)R) is an ATP-gated ion channel and its spinal up-regulation has been found to be crucial for the development of neuropathic pain following peripheral nerve injury. The initiation of mechanical allodynia in rat EAN was observed at day 9 before the onset of neurological signs. Maximal level of mechanical allodynia was observed from days 17-19 and then a slow recovery, long after the cessation of typical neurological signs of EAN, until day 37 was observed. Expression of P2X(4)R in lumbar spinal cords was studied by immunohistochemistry. P2X(4)R immunoreactivity (IR) was mainly seen in gray matter, particularly in the dorsal horn. Accumulation of P2X(4)R(+) cells in the lumbar dorsal horn was observed at day 9, reached the maximal level at day 17 and remained elevated until day 37 after immunization. Furthermore, a negative correlation between the density of P2X(4)R(+) cells in the lumbar dorsal horn with mean hind-paw withdrawal threshold in EAN rats was seen, indicating that P2X(4)R might contribute to EAN mechanical allodynia. Double staining revealed that almost all P2X(4)R(+) cells co-expressed CD68, a marker for reactive microglia, but not the astrocyte marker, glial fibrillary acidic protein (GFAP). Our data demonstrate that EAN induces mechanical allodynia and P2X(4)R expression in spinal microglia, suggesting that EAN is a good animal model for neuropathic pain in polyneuropathy and spinal microglia activation might participate in EAN-induced neuropathic pain.
实验性自身免疫性神经炎(EAN)是急性炎症性脱髓鞘性多发性神经根神经病(AIDP)的动物模型,AIDP是吉兰-巴雷综合征(GBS)最常见的亚型。虽然神经性疼痛是GBS的常见症状,但其潜在机制仍不清楚。中枢敏化,特别是脊髓胶质细胞(小胶质细胞和星形胶质细胞)的激活,对神经性疼痛的起始和维持很重要。P2X(4)受体(P2X(4)R)是一种ATP门控离子通道,其在脊髓中的上调已被发现对周围神经损伤后神经性疼痛的发展至关重要。在大鼠EAN中,在神经体征出现前第9天观察到机械性异常性疼痛的起始。在第17 - 19天观察到机械性异常性疼痛的最大程度,然后在EAN典型神经体征停止很久之后,直到第37天观察到缓慢恢复。通过免疫组织化学研究腰段脊髓中P2X(4)R的表达。P2X(4)R免疫反应性(IR)主要见于灰质,特别是背角。在免疫后第9天观察到腰段背角中P2X(4)R(+)细胞的聚集,在第17天达到最大水平,并一直升高到第37天。此外,在EAN大鼠中,腰段背角中P2X(4)R(+)细胞的密度与平均后爪撤离阈值之间存在负相关,表明P2X(4)R可能导致EAN的机械性异常性疼痛。双重染色显示,几乎所有P2X(4)R(+)细胞共表达CD68,这是反应性小胶质细胞的标志物,但不表达星形胶质细胞标志物胶质纤维酸性蛋白(GFAP)。我们的数据表明,EAN诱导脊髓小胶质细胞中的机械性异常性疼痛和P2X(4)R表达,提示EAN是多神经病中神经性疼痛的良好动物模型,并且脊髓小胶质细胞激活可能参与EAN诱导的神经性疼痛。
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