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Pharmacogenetics of multiple sclerosis: personalized therapy with immunomodulatory drugs

机译:多发性硬化症的药物发生:免疫调节药物的个性化疗法

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Pharmacogenetic (PG) studies aim to discover the individual genetic background that underlies the heterogeneity of treatment response, and thus find biomarkers for identification of individual patients who will benefit the most from the therapy administered or urgently require the alternate drug. Over the last decade, PG studies have made progress in terms of multiple sclerosis (MS), which is one of the most severe neurodegenerative diseases of the central nervous system. With the understanding of the role of the immune system in the pathogenesis of MS, a number of immunomodulatory drugs were developed for MS treatment management. However, clinical response to these disease-modifying therapies varies in individual patients. Interferon-beta and glatiramer acetate showed the most reliable long-term safety and remain among the first-line disease-modifying therapies for MS worldwide. Here, we will review the results of interferon-beta and glatiramer acetate PG studies with a detailed analysis of study design and approaches, their advantages and limitations, and future perspectives.
机译:药物发生(PG)研究旨在发现个体遗传背景,使治疗反应的异质性提升,从而找到生物标志物,用于鉴定将受益于施用或迫切需要替代药物的治疗中最多的个体患者。在过去十年中,PG研究就多发性硬化症(MS)进行了进展,这是中枢神经系统中最严重的神经变性疾病之一。通过了解免疫系统在MS发病机制中的作用,为MS治疗管理开发了许多免疫调节药物。然而,对这些疾病改性治疗的临床反应在个体患者中变化。干扰素 - β和Glatiramer醋酸酯显示出最可靠的长期安全性,并留在全球MS的一线疾病修饰疗法中。在这里,我们将审查干扰素-β和Glatiramer醋酸酯PG研究的结果,并详细分析研究设计和方法,优势和局限以及未来的观点。

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