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Predicting responders to therapies for multiple sclerosis.

机译:预测对多发性硬化症疗法的反应者。

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摘要

Therapies for relapsing-remitting multiple sclerosis (RRMS) are only partially effective, and, in most patients receiving such treatment, clinical activity persists. Accurately assessing the treatment response to disease-modifying agents enables non-responder patients to be identified at an early stage into therapy. Patients can then be switched to another, potentially more effective, therapy before too much neurological damage has occurred. Several criteria based on relapses, disability progression or both have been proposed for clinical evaluation of the treatment response to disease-modifying agents. These criteria have not been independently validated, however, and no consensus over which are the best to use currently exists among investigators. MRI can also be employed to detect disease activity in patients treated with disease-modifying agents. Changes on MRI can provide subclinical data relating to disease activity that can be of great benefit in patients monitoring, as inflammatory events occur more often than clinical events. Pharmacogenomic approaches are in the early stages of development for MS, but hold great promise for the eventual development of individually tailored therapies. In this Review, we discuss the proposed approaches for monitoring and predicting treatment responses to disease-modifying agents in patients with RRMS. We evaluate the roles of clinical measures, MRI and pharmacogenomics in these processes.
机译:复发缓解型多发性硬化症(RRMS)的治疗仅部分有效,并且在接受这种治疗的大多数患者中,临床活动持续存在。准确评估对疾病改良剂的治疗反应,可以在治疗的早期阶段识别出无反应的患者。然后,在发生过多的神经损伤之前,可以将患者转到另一种可能更有效的治疗方法。已经提出了几种基于复发,残疾发展或两者的标准来对疾病改变剂的治疗反应进行临床评估。但是,这些标准尚未得到独立验证,研究人员之间目前尚无共识。 MRI还可以用于检测用疾病改良剂治疗的患者的疾病活动。 MRI的变化可以提供与疾病活动有关的亚临床数据,这在患者监测中可能会大有裨益,因为炎症事件比临床事件更经常发生。药物基因组学方法尚处于MS研发的早期阶段,但有望最终开发出个性化的疗法。在本综述中,我们讨论了用于监视和预测RRMS患者对疾病改变剂的治疗反应的拟议方法。我们评估在这些过程中临床措施,MRI和药物基因组学的作用。

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