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首页> 外文期刊>Degenerative Neurological and Neuromuscular Disease >Identifying responders and nonresponders to interferon therapy in multiple sclerosis
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Identifying responders and nonresponders to interferon therapy in multiple sclerosis

机译:识别多发性硬化症中干扰素治疗的反应者和非反应者

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Abstract: Interferon beta is a well established disease-modifying agent used for relapsing-remitting multiple sclerosis. Despite treatment, a relevant proportion of patients continue to experience clinical (ie, relapses, worsening of disability) and magnetic resonance imaging (MRI) activity. Early identification of responders and nonresponders to interferon beta is strongly recommended to select patients who need a prompt switch to another disease-modifying agent and to ultimately avoid accumulation of fixed disability over time. Detecting responders and nonresponders to interferon beta can be challenging, mainly because of the lack of a clear and shared clinical definition of response to treatment. Clinical features at the start of treatment should be considered as prognostic factors, but MRI parameters assessed during treatment, such as contrast-enhancing lesions or new T2-hyperintense lesions, may be sensitive markers of response to interferon beta. Quantitative scoring systems derived from a combination of relapses and MRI activity have recently been proposed as practical tools for use in the everyday clinical setting. Blood biomarkers, such as neutralizing antibodies to interferon beta and Myxovirus resistance protein A, provide further useful information for detecting responders and nonresponders to interferon beta. However, since the presence of neutralizing antibodies can only partially explain the nonresponse to interferon beta, biomarkers of interferon beta activity possibly related to the pathogenesis of the disease could represent a future step toward a tailored, long-lasting effective treatment against multiple sclerosis.
机译:摘要:干扰素β是一种完善的疾病缓解剂,用于复发缓解型多发性硬化症。尽管进行了治疗,仍有相当一部分患者继续经历临床(即复发,残疾加重)和磁共振成像(MRI)活动。强烈建议及早识别对干扰素β的反应者和无反应者,以选择需要立即改用另一种疾病改良剂并最终避免因长期积累而导致的固定残疾的患者。检测对干扰素β的反应者和非反应者可能具有挑战性,主要是因为缺乏对治疗反应的明确且共有的临床定义。治疗开始时的临床特征应被视为预后因素,但是在治疗过程中评估的MRI参数(例如对比增强病灶或新的T2高强度病灶)可能是对干扰素β反应的敏感标志物。最近已经提出了将复发和MRI活性相结合的定量评分系统,作为在日常临床环境中使用的实用工具。血液生物标志物,例如抗干扰素β和粘液病毒抗性蛋白A的中和抗体,为检测干扰素β的应答者和非应答者提供了更多有用的信息。但是,由于中和抗体的存在只能部分解释对干扰素β的无反应,因此可能与疾病发病机理有关的干扰素β活性的生物标志物可能代表着朝着针对多发性硬化症进行定制,长期有效治疗的未来一步。

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