Department of Molecular Cell Biology and Immunology, Amsterdam UMC, location Vrije Universiteit Amsterdam, De Boelelaan 1117, Amsterdam, The Netherlands.
MS Center Amsterdam, Amsterdam UMC, location VU Medical Center, Amsterdam, The Netherlands.
J Neuroinflammation. 2024 Jan 17;21(1):21. doi: 10.1186/s12974-023-02981-w.
Multiple sclerosis (MS) is a chronic autoimmune disease of the central nervous system (CNS), characterized by neuroinflammation, demyelination, and neurodegeneration. Considering the increasing prevalence among young adults worldwide and the disabling phenotype of the disease, a deeper understanding of the complexity of the disease pathogenesis is needed to ultimately improve diagnosis and personalize treatment opportunities. Recent findings suggest that bioactive lipid mediators (LM) derived from ω-3/-6 polyunsaturated fatty acids (PUFA), also termed eicosanoids, may contribute to MS pathogenesis. For example, disturbances in LM profiles and especially those derived from the ω-6 PUFA arachidonic acid (AA) have been reported in people with MS (PwMS), where they may contribute to the chronicity of neuroinflammatory processes. Moreover, we have previously shown that certain AA-derived LMs also associated with neurodegenerative processes in PwMS, suggesting that AA-derived LMs are involved in more pathological events than solely neuroinflammation. Yet, to date, a comprehensive overview of the contribution of these LMs to MS-associated pathological processes remains elusive.
This review summarizes and critically evaluates the current body of literature on the eicosanoid biosynthetic pathway and its contribution to key pathological hallmarks of MS during different disease stages. Various parts of the eicosanoid pathway are highlighted, namely, the prostanoid, leukotriene, and hydroxyeicosatetraenoic acids (HETEs) biochemical routes that include specific enzymes of the cyclooxygenases (COXs) and lipoxygenases (LOX) families. In addition, cellular sources of LMs and their potential target cells based on receptor expression profiles will be discussed in the context of MS. Finally, we propose novel therapeutic approaches based on eicosanoid pathway and/or receptor modulation to ultimately target chronic neuroinflammation, demyelination and neurodegeneration in MS.
The eicosanoid pathway is intrinsically linked to specific aspects of MS pathogenesis. Therefore, we propose that novel intervention strategies, with the aim of accurately modulating the eicosanoid pathway towards the biosynthesis of beneficial LMs, can potentially contribute to more patient- and MS subtype-specific treatment opportunities to combat MS.
多发性硬化症(MS)是一种中枢神经系统(CNS)的慢性自身免疫性疾病,其特征为神经炎症、脱髓鞘和神经退行性变。考虑到全球范围内年轻人中发病率的增加和疾病致残的表型,需要更深入地了解疾病发病机制的复杂性,以最终改善诊断和实现个体化治疗机会。最近的研究结果表明,来源于 ω-3/-6 多不饱和脂肪酸(PUFA)的生物活性脂质介质(LM),也称为类二十烷酸,可能有助于 MS 的发病机制。例如,在多发性硬化症患者(PwMS)中已经报道了 LM 谱的紊乱,特别是来源于 ω-6 PUFA 花生四烯酸(AA)的 LM 谱紊乱,它们可能导致神经炎症过程的慢性化。此外,我们之前已经表明,某些 AA 衍生的 LM 也与 PwMS 中的神经退行性过程有关,这表明 AA 衍生的 LM 参与的病理事件不仅仅是神经炎症。然而,迄今为止,关于这些 LM 对 MS 相关病理过程的贡献的全面概述仍难以捉摸。
本综述总结并批判性地评估了目前关于类二十烷酸生物合成途径及其在不同疾病阶段对多发性硬化症关键病理特征的贡献的文献。突出了类二十烷酸途径的各个部分,即前列腺素、白三烯和羟二十碳四烯酸(HETEs)生化途径,包括环加氧酶(COXs)和脂加氧酶(LOXs)家族的特定酶。此外,将根据受体表达谱讨论 LM 的细胞来源及其潜在的靶细胞在多发性硬化症中的情况。最后,我们提出了基于类二十烷酸途径和/或受体调节的新的治疗方法,以最终针对多发性硬化症中的慢性神经炎症、脱髓鞘和神经退行性变。
类二十烷酸途径与多发性硬化症发病机制的特定方面密切相关。因此,我们提出,旨在准确调节类二十烷酸途径以合成有益 LM 的新干预策略,可能有助于针对更多的患者和多发性硬化症亚型特异性的治疗机会来对抗多发性硬化症。
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