Institute of Neuroscience, Zhejiang University School of Medicine Hangzhou, China.
Department of Obstetrics and Gyneocology, Hangzhou Red Cross Hospital Hangzhou, China.
Front Neuroanat. 2013 Dec 30;7:44. doi: 10.3389/fnana.2013.00044. eCollection 2013.
Experimentalallergic encephalomyelitis (EAE) is an animal model for inflammatory demyelinating autoimmune disease, i.e., multiple sclerosis (MS). In the present study, we investigated the antineuroinflammatory/neuroprotective effects of C16, an ανβ3 integrin-binding peptide, and recombinant rat ciliary neurotrophic factor (CNTF), a cytokine that was originally identified as a survival factor for neurons, in an acute rodent EAE model. In this model, C16 peptide was injected intravenously every day for 2 weeks, and CNTF was delivered into the cerebral ventricles with Alzet miniosmotic pumps. Disease severity was assessed weekly using a scale ranging from 0 to 5. Multiple histological and molecular biological assays were employed to assess inflammation, axonal loss, neuronal apoptosis, white matter demyelination, and gliosis in the brain and spinal cord of different groups. Our results showed that the EAE induced rats revealed a significant increase in inflammatory cells infiltration, while C16 treatment could inhibit the infiltration of leukocytes and macrophages down to 2/3-1/3 of vehicle treated EAE control (P < 0.05). The delayed onset of disease, reduced clinical score (P < 0.01) in peak stage and more rapid recovery also were achieved in C16 treated group. Besides impairing inflammation, CNTF treatment also exerted direct neuroprotective effects, decreasing demyelination and axon loss score (P < 0.05 versus vehicle treated EAE control), and reducing the neuronal death from 40 to 50% to 10 to 20% (P < 0.05). Both treatments suppressed the expression of cytokine tumor necrosis factor-α and interferon-γ when compared with the vehicle control (P < 0.05). Combined treatment with C16 and CNTF produced more obvious functional recovery and neuroprotective effects than individually treatment (P < 0.05). These results suggested that combination treatment with C16 and CNTF, which target different neuroprotection pathways, may be an effective therapeutic alternative to traditional therapy.
实验性变态反应性脑脊髓炎 (EAE) 是一种炎症性脱髓鞘自身免疫性疾病的动物模型,即多发性硬化症 (MS)。在本研究中,我们研究了 C16,一种ανβ3 整合素结合肽,和重组大鼠睫状神经营养因子 (CNTF),一种最初被鉴定为神经元存活因子的细胞因子,在急性啮齿动物 EAE 模型中的神经抗炎/神经保护作用。在该模型中,C16 肽每天静脉注射 2 周,CNTF 通过 Alzet 迷你渗透泵递送到脑室。每周使用 0 到 5 的量表评估疾病严重程度。采用多种组织学和分子生物学方法评估不同组脑和脊髓中的炎症、轴突丢失、神经元凋亡、白质脱髓鞘和神经胶质增生。我们的结果表明,EAE 诱导的大鼠显示出白细胞和巨噬细胞浸润的显著增加,而 C16 治疗可将白细胞和巨噬细胞的浸润抑制至对照组的 2/3-1/3(P < 0.05)。C16 治疗组还可延迟疾病发作,在高峰期降低临床评分(P < 0.01),并更快恢复。除了损害炎症外,CNTF 治疗还发挥了直接的神经保护作用,降低脱髓鞘和轴突丢失评分(P < 0.05 与对照组相比),并将神经元死亡从 40%至 50%降低至 10%至 20%(P < 0.05)。与对照组相比,两种治疗方法均降低了细胞因子肿瘤坏死因子-α和干扰素-γ的表达(P < 0.05)。与单独治疗相比,C16 和 CNTF 的联合治疗产生了更明显的功能恢复和神经保护作用(P < 0.05)。这些结果表明,针对不同神经保护途径的 C16 和 CNTF 的联合治疗可能是传统治疗的有效替代方法。
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