Peroxiredoxin 6 Alone or in Combination with Fingolimod Ameliorates EAE.

IF 4.8 2区医学 Q1 NEUROSCIENCES

Current Neuropharmacology Pub Date : 2025-07-07 DOI:10.2174/011570159X372166250619064636

Lunin S M, Novoselova E G, Glushkova O V, Parfenyuk S B, Kuzekova A A, Novoselova T V, Sharapov M G, Mubarakshina E K, Goncharov R G, Khrenov M O

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引用次数: 0

Abstract

Introduction: Multiple Sclerosis (MS) is characterized by the infiltration of leukocytes into the nervous tissue, and disruption of the Blood-Brain Barrier (BBB) is one of the main factors in the progression of MS and its model, Experimental Autoimmune Encephalomyelitis (EAE). Furthermore, some anti-lymphocytic drugs against MS may inherently produce BBB disruption as their side effect. This study hypothesized that drugs restoring the BBB may be useful for the treatment of MS and EAE, as well as for ameliorating the side effects of modern anti-lymphocytic drugs.

Methods: EAE was induced in SJL/J mice. EAE progression was evaluated by a severity score and a plasma cytokine profile, while a BBB condition was evaluated by the Evans dye method, Tight Junction Proteins (TJPs) content, and leukocyte infiltration.

Results: The mice with EAE demonstrated neurological symptoms, a cytokine response, and BBB deterioration, which was associated with upregulation of the NADPH oxidases NOX1 and NOX4 in the brain. Administration of the anti-lymphocyte drug fingolimod to EAE mice caused lymphopenia, improved animal health, enhanced the BBB function during the administration period, and decreased the pro-inflammatory response, but it was accompanied by a "withdrawal effect," defined as a sharp increase in the IL-17 and IFN-gamma to levels higher than those in untreated animals, lymphocyte hyperactivation, worsening symptoms, and increasing BBB permeability after discontinuation of fingolimod. Administration of peroxiredoxin 6 (Prdx6) to EAE mice also improved BBB, decreased lymphocyte infiltration and NADPH oxidase expression, and ameliorated symptoms. Preliminary administration of Prdx6 before the fingolimod treatment eliminated the "withdrawal effect" of fingolimod and led to full recovery of the EAE mice. This Prdx6 effect was associated with the activation of anti-proliferative and pro-apoptotic signaling cascades in lymphocytes.

Discussion and conclusion: Both fingolimod and Prdx6 produced beneficial effects, while Prdx6 may be useful for ameliorating the side effects of anti-lymphocytic drugs. Accounting for literature data that discontinuation of MS treatment is very likely to lead to a severe MS rebound, a drug that prevents the rebound should be useful.

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过氧还蛋白6单用或联用芬戈莫德可改善EAE。

简介：多发性硬化症（Multiple Sclerosis， MS）以白细胞向神经组织浸润为特征，血脑屏障（Blood-Brain Barrier， BBB）的破坏是MS及其模型实验性自身免疫性脑脊髓炎（Experimental Autoimmune Encephalomyelitis， EAE）进展的主要因素之一。此外，一些抗淋巴细胞药物可能固有地产生血脑屏障破坏作为其副作用。本研究假设恢复血脑屏障的药物可能有助于治疗MS和EAE，以及改善现代抗淋巴细胞药物的副作用。方法：对SJL/J小鼠进行EAE诱导。通过严重程度评分和血浆细胞因子谱来评估EAE的进展，而通过Evans染色法、紧密连接蛋白（TJPs）含量和白细胞浸润来评估BBB状况。结果：EAE小鼠表现出神经系统症状、细胞因子反应和血脑屏障恶化，这与脑内NADPH氧化酶NOX1和NOX4的上调有关。给EAE小鼠服用抗淋巴细胞药物fingolimod导致淋巴细胞减少，改善了动物健康，在给药期间增强了血脑屏障功能，减少了促炎反应，但它伴随着“停药效应”，定义为IL-17和ifn - γ急剧增加到高于未治疗动物的水平，淋巴细胞过度激活，症状恶化，停药后血脑屏障通透性增加。给予EAE小鼠过氧化物还蛋白6 （Prdx6）也能改善血脑屏障，降低淋巴细胞浸润和NADPH氧化酶表达，改善症状。在给药前先给药Prdx6可消除芬戈莫德的“戒断效应”，使EAE小鼠完全恢复。这种Prdx6效应与淋巴细胞中抗增殖和促凋亡信号级联的激活有关。讨论与结论：芬戈莫德和Prdx6均有有益作用，而Prdx6可能有助于改善抗淋巴细胞药物的副作用。考虑到文献资料显示停止多发性硬化症治疗很可能导致严重的多发性硬化症反弹，一种防止反弹的药物应该是有用的。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Current Neuropharmacology 医学-神经科学

CiteScore

8.70

自引率

1.90%

发文量

369

审稿时长

>12 weeks

期刊介绍： Current Neuropharmacology aims to provide current, comprehensive/mini reviews and guest edited issues of all areas of neuropharmacology and related matters of neuroscience. The reviews cover the fields of molecular, cellular, and systems/behavioural aspects of neuropharmacology and neuroscience. The journal serves as a comprehensive, multidisciplinary expert forum for neuropharmacologists and neuroscientists.