Department of Neurology, Section of Developmental Neurobiology, University Hospital Wuerzburg, D-97080, Wuerzburg, Germany.
J Neuroinflammation. 2018 Jul 3;15(1):194. doi: 10.1186/s12974-018-1228-z.
Genetically caused neurological disorders of the central nervous system (CNS) are mostly characterized by poor or even fatal clinical outcome and few or no causative treatments are available. Often, these disorders are associated with low-grade, disease-promoting inflammation, another feature shared by progressive forms of multiple sclerosis (PMS). We previously generated two mouse lines carrying distinct mutations in the oligodendrocytic PLP1 gene that have initially been identified in patients diagnosed with MS. These mutations cause a loss of PLP function leading to a histopathological and clinical phenotype common to both PMS and genetic CNS disorders, like hereditary spastic paraplegias. Importantly, neuroinflammation promotes disease progression in these models, suggesting that pharmacological modulation of inflammation might ameliorate disease outcome.
We applied teriflunomide, an approved medication for relapsing-remitting MS targeting activated T-lymphocytes, in the drinking water (10 mg/kg body weight/day). Experimental long-term treatment of PLP mutant mice was non-invasively monitored by longitudinal optical coherence tomography and by rotarod analysis. Immunomodulatory effects were subsequently analyzed by flow cytometry and immunohistochemistry and treatment effects regarding neural damage, and neurodegeneration were assessed by histology and immunohistochemistry.
Preventive treatment with teriflunomide attenuated the increase in number of CD8+ cytotoxic effector T cells and fostered the proliferation of CD8+ CD122+ PD-1+ regulatory T cells in the CNS. This led to an amelioration of axonopathic features and neuron loss in the retinotectal system, also reflected by reduced thinning of the innermost retinal composite layer in longitudinal studies and ameliorated clinical outcome upon preventive long-term treatment. Treatment of immune-incompetent PLP mutants did not provide evidence for a direct, neuroprotective effect of the medication. When treatment was terminated, no rebound of neuroinflammation occurred and histopathological improvement was preserved for at least 75 days without treatment. After disease onset, teriflunomide halted ongoing axonal perturbation and enabled a recovery of dendritic arborization by surviving ganglion cells. However, neither neuron loss nor clinical features were ameliorated, likely due to already advanced neurodegeneration before treatment onset.
We identify teriflunomide as a possible medication not only for PMS but also for inflammation-related genetic diseases of the nervous system for which causal treatment options are presently lacking.
中枢神经系统(CNS)的遗传神经病变主要表现为预后不良甚至致命,且目前可用的治疗方法很少或没有。这些疾病通常与低度、促病性炎症相关,而进展性多发性硬化症(PMS)也具有这一特征。我们之前生成了两种携带少突胶质细胞 PLP1 基因不同突变的小鼠系,这些突变最初在被诊断为 MS 的患者中被发现。这些突变导致 PLP 功能丧失,导致 PMS 和遗传性 CNS 疾病(如遗传性痉挛性截瘫)的组织病理学和临床表型共同出现。重要的是,神经炎症会促进这些模型中的疾病进展,表明炎症的药物调节可能会改善疾病结果。
我们将特立氟胺(一种用于治疗复发缓解型多发性硬化症的已批准药物,针对活化的 T 淋巴细胞)应用于饮用水中(10mg/kg 体重/天)。通过纵向光学相干断层扫描和旋转棒分析,非侵入性地监测 PLP 突变小鼠的长期实验治疗。随后通过流式细胞术和免疫组织化学分析免疫调节作用,并通过组织学和免疫组织化学评估神经损伤和神经退行性变的治疗效果。
特立氟胺的预防性治疗减轻了 CD8+细胞毒性效应 T 细胞数量的增加,并促进了 CNS 中 CD8+ CD122+ PD-1+调节性 T 细胞的增殖。这导致光感受器-视网膜系统中的轴突病变特征和神经元丢失得到改善,纵向研究中也反映为最内层视网膜复合层变薄减少,预防性长期治疗后的临床结果得到改善。免疫功能低下的 PLP 突变体的治疗并未提供药物直接神经保护作用的证据。停止治疗时,神经炎症没有反弹,在没有治疗的情况下,组织病理学改善至少可维持 75 天。疾病发作后,特立氟胺停止了进行中的轴突扰动,并使存活的神经节细胞的树突分支恢复。然而,神经元丢失或临床特征都没有得到改善,这可能是由于在治疗开始前已经出现了晚期神经退行性变。
我们将特立氟胺确定为一种可能的药物,不仅可用于 PMS,还可用于目前尚无病因治疗方法的与炎症相关的遗传性神经系统疾病。
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