Department of Neurology, Heinrich-Heine University, Düsseldorf, Germany.
CNS Drugs. 2011 Jun 1;25(6):491-502. doi: 10.2165/11591110-000000000-00000.
Multiple sclerosis (MS) is characterized by autoimmune inflammation and subsequent neurodegeneration. It is believed that early in the disease course, proinflammatory T cells that are activated in the periphery by antigen presentation cross the blood-brain barrier (BBB) into the CNS directed by various chemotaxic agents. However, to date, there has been no formal demonstration of a specific precipitating antigen. Once inside the CNS, activated T cells including T helper-1 (T(h)1), T(h)17, γδ and CD8+ types are believed to secrete proinflammatory cytokines. Decreased levels of T(h)2 cells also correlate with relapses and disease progression in MS, since T(h)2-derived cytokines are predominantly anti-inflammatory. In healthy tissue, inflammatory effects are opposed by specific subsets of regulatory T cells (T(regs)) including CD4+, CD25+ and FoxP3+ cells that have the ability to downregulate the activity of proinflammatory T cells, allowing repair and recovery to generally follow inflammatory insult. Given their function, the pathogenesis of MS most likely involves deficits of T(reg) function, which allow autoimmune inflammation and resultant neurodegeneration to proceed relatively unchecked. Interferons (IFNs) are naturally occurring cytokines possessing a wide range of anti-inflammatory properties. Recombinant forms of IFNβ are widely used as first-line treatment in relapsing forms of MS. The mechanism of action of IFNβ is complex, involving effects at multiple levels of cellular function. IFNβ appears to directly increase expression and concentration of anti-inflammatory agents while downregulating the expression of proinflammatory cytokines. IFNβ treatment may reduce the trafficking of inflammatory cells across the BBB and increase nerve growth factor production, leading to a potential increase in neuronal survival and repair. IFNβ can also increase the number of CD56bright natural killer cells in the peripheral blood. These cells are efficient producers of anti-inflammatory mediators, and may have the ability to curb neuron inflammation. The mechanistic effects of IFNβ manifest clinically as reduced MRI lesion activity, reduced brain atrophy, increased time to reach clinically definite MS after the onset of neurological symptoms, decreased relapse rate and reduced risk of sustained disability progression. The mechanism of action of IFNβ in MS is multifactorial and incompletely understood. Ongoing and future studies will increase our understanding of the actions of IFNβ on the immune system and the CNS, which will in turn aid advances in the management of MS.
多发性硬化症(MS)的特征是自身免疫炎症和随后的神经退行性变。据信,在疾病早期,在外周被抗原呈递激活的促炎 T 细胞通过各种趋化因子导向穿过血脑屏障(BBB)进入中枢神经系统。然而,迄今为止,还没有正式证明存在特定的触发抗原。一旦进入中枢神经系统,包括辅助性 T 细胞 1(T(h)1)、T(h)17、γδ和 CD8+型在内的激活 T 细胞被认为会分泌促炎细胞因子。MS 患者的 T(h)2 细胞水平降低也与复发和疾病进展相关,因为 T(h)2 衍生的细胞因子主要具有抗炎作用。在健康组织中,炎症效应被特定的调节性 T 细胞(T(regs))亚群所拮抗,包括 CD4+、CD25+和 FoxP3+细胞,它们具有下调促炎 T 细胞活性的能力,从而允许修复和恢复通常在炎症损伤后进行。鉴于它们的功能,MS 的发病机制很可能涉及 T(regs)功能缺陷,这使得自身免疫炎症和由此产生的神经退行性变相对不受控制。干扰素(IFN)是具有广泛抗炎特性的天然细胞因子。重组形式的 IFNβ 被广泛用作复发性 MS 的一线治疗药物。IFNβ 的作用机制复杂,涉及细胞功能的多个层面的影响。IFNβ 似乎直接增加抗炎剂的表达和浓度,同时下调促炎细胞因子的表达。IFNβ 治疗可减少炎症细胞穿过 BBB 的迁移,并增加神经生长因子的产生,从而导致神经元存活和修复的潜在增加。IFNβ 还可以增加外周血中 CD56bright 自然杀伤细胞的数量。这些细胞是抗炎介质的有效产生者,并且可能具有抑制神经元炎症的能力。IFNβ 的临床作用表现为 MRI 病变活动减少、脑萎缩减少、神经症状出现后达到临床确诊 MS 的时间延长、复发率降低和持续残疾进展风险降低。IFNβ 在 MS 中的作用机制是多因素的,目前尚不完全清楚。正在进行和未来的研究将增加我们对 IFNβ 对免疫系统和中枢神经系统的作用的理解,这反过来将有助于 MS 管理的进展。
