Department of Neuroimmunology, Medical University Vienna, Center for Brain Research, Spitalgasse 4, Vienna, A-1090, Austria.
Acta Neuropathol Commun. 2013 May 8;1:5. doi: 10.1186/2051-5960-1-5.
Neuromyelitis optica (NMO) is a severe, disabling disease of the central nervous system (CNS) characterized by the formation of astrocyte-destructive, neutrophil-dominated inflammatory lesions in the spinal cord and optic nerves. These lesions are initiated by the binding of pathogenic aquaporin 4 (AQP4)-specific autoantibodies to astrocytes and subsequent complement-mediated lysis of these cells. Typically, these lesions form in a setting of CNS inflammation, where the blood-brain barrier is open for the entry of antibodies and complement. However, it remained unclear to which extent pro-inflammatory cytokines and chemokines contribute to the formation of NMO lesions. To specifically address this question, we injected the cytokines interleukin-1 beta, tumor necrosis factor alpha, interleukin-6, interferon gamma and the chemokine CXCL2 into the striatum of NMO-IgG seropositive rats and analyzed the tissue 24 hours later by immunohistochemistry.
All injected cytokines and chemokines led to profound leakage of immunoglobulins into the injected hemisphere, but only interleukin-1 beta induced the formation of perivascular, neutrophil-infiltrated lesions with AQP4 loss and complement-mediated astrocyte destruction distant from the needle tract. Treatment of rat brain endothelial cells with interleukin-1 beta, but not with any other cytokine or chemokine applied at the same concentration and over the same period of time, caused profound upregulation of granulocyte-recruiting and supporting molecules. Injection of interleukin-1 beta caused higher numbers of blood vessels with perivascular, cellular C1q reactivity than any other cytokine tested. Finally, the screening of a large sample of CNS lesions from NMO and multiple sclerosis patients revealed large numbers of interleukin-1 beta-reactive macrophages/activated microglial cells in active NMO lesions but not in MS lesions with comparable lesion activity and location.
Our data strongly suggest that interleukin-1 beta released in NMO lesions and interleukin-1 beta-induced production/accumulation of complement factors (like C1q) facilitate neutrophil entry and BBB breakdown in the vicinity of NMO lesions, and might thus be an important secondary factor for lesion formation, possibly by paving the ground for rapid lesion growth and amplified immune cell recruitment to this site.
视神经脊髓炎(NMO)是一种严重的中枢神经系统(CNS)疾病,其特征是在脊髓和视神经中形成星形胶质细胞破坏性、中性粒细胞占主导的炎症性病变。这些病变是由致病性水通道蛋白 4(AQP4)特异性自身抗体与星形胶质细胞结合,随后补体介导这些细胞溶解引起的。通常,这些病变是在中枢神经系统炎症的情况下形成的,此时血脑屏障对抗体和补体的进入是开放的。然而,细胞因子和趋化因子在多大程度上促进 NMO 病变的形成仍不清楚。为了专门解决这个问题,我们将细胞因子白细胞介素 1β、肿瘤坏死因子-α、白细胞介素 6、干扰素 γ和趋化因子 CXCL2 注射到 NMO-IgG 阳性大鼠的纹状体中,并在 24 小时后通过免疫组织化学进行分析。
所有注射的细胞因子和趋化因子都导致免疫球蛋白大量渗漏到注射的半球,但只有白细胞介素 1β诱导了血管周围、中性粒细胞浸润的病变形成,伴有 AQP4 丢失和补体介导的星形胶质细胞破坏,远离针道。与任何其他细胞因子或趋化因子在相同浓度和相同时间内应用于大鼠脑内皮细胞相比,白细胞介素 1β的治疗导致粒细胞募集和支持分子的显著上调。与测试的任何其他细胞因子相比,白细胞介素 1β注射导致更多的血管出现血管周围、细胞性 C1q 反应性。最后,对来自 NMO 和多发性硬化症患者的大量 CNS 病变进行筛选,发现大量白细胞介素 1β反应性巨噬细胞/激活的小胶质细胞存在于活动期 NMO 病变中,但不存在于具有相似病变活动和位置的 MS 病变中。
我们的数据强烈表明,NMO 病变中释放的白细胞介素 1β和白细胞介素 1β诱导的补体因子(如 C1q)的产生/积累有助于中性粒细胞进入和 NMO 病变附近的血脑屏障破裂,因此可能是病变形成的一个重要的次要因素,可能通过为快速病变生长和增强免疫细胞募集到该部位铺平道路。
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