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首页> 外文期刊>Journal of neurology >The combination of cyclophosphamide plus interferon beta as rescue therapy could be used to treat relapsing-remitting multiple sclerosis patients Twenty-four months follow-up.
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The combination of cyclophosphamide plus interferon beta as rescue therapy could be used to treat relapsing-remitting multiple sclerosis patients Twenty-four months follow-up.

机译:环磷酰胺加干扰素β联合作为抢救疗法可用于治疗复发缓解型多发性硬化症患者二十四个月的随访。

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The aim of the present study was to evaluate the efficacy of the combination of cyclophosphamide (CTX) and interferon beta (IFN beta) in a group of relapsing remitting (RR) multiple sclerosis (MS) patients who experienced treatment failure during IFN beta therapy. It is the general experience that immunomodulatory agents (IMA) are only partially effective in RR patients. Recent data on the efficacy of immunosuppressive therapies for these patients are encouraging. The anti-inflammatory and immunosuppressive effects of CTX have been utilized to treat selected cases of multiple sclerosis with a progressive and worsening course as rescue therapy. Thirty RR MS patients with clinically defined MS who experienced treatment failure during IFN beta therapy (2 or more relapses per year or 1.5 EDSS point worsening in one year) were enrolled in the study and treated with CTX iv pulse therapy added to IFN beta and followed up for 24 months. As primary endpoints we evaluated the yearly relapse rate. We also evaluated the percentage of patients free of relapses and of EDSS variations. We analysed the results at one year before entry (T0: IFN beta alone), 12 (T1) and 24 (T2) months after entry. Brain MRI was performed at T0, at T1 and T2. The 30 RR patients who had experienced a high number of relapses (r r =1.4) at T0 showed a significant improvement in yearly relapse rate (rr = 0.4) at T1 and a further improvement (rr = 0.17) at T2 (p < 0.001). The percentage of patients free of relapse was 70% at T2 (p < 0.0001). EDSS score changed from 2.6+/-1.23 at T0 to 2.2 +/- 1.5 at T2, showing only a trend of improvement.No significant variation of MRI lesion load and no severe adverse events were recorded during the study. These data showed that the combination of CTX plus IFN beta halted the progression of disease in active and deteriorating MS patients suggesting the necessity of RCTs to test the efficacy of this combination therapy in active RRMS patients or in patients who experienced treatment failure in response todisease modifying drugs (DMDs).
机译:本研究的目的是评估环磷酰胺(CTX)和干扰素beta(IFN beta)的组合对一组在IFN beta治疗期间出现治疗失败的复发缓解(RR)多发性硬化症(MS)患者的疗效。一般经验是免疫调节剂(IMA)在RR患者中仅部分有效。关于这些患者的免疫抑制疗法功效的最新数据令人鼓舞。 CTX的抗炎和免疫抑制作用已被用于治疗多发性硬化症的选定病例,其进展和恶化过​​程作为抢救疗法。纳入研究的30名RR MS患者在临床上定义为MS,他们在IFNβ治疗期间出现治疗失败(每年复发2次或以上,或一年中恶化EDSS 1.5分),并在IFNβ中加入CTX iv脉冲治疗长达24个月。作为主要终点,我们评估了年复发率。我们还评估了无复发和EDSS变异的患者百分比。我们分析了进入前一年(T0:仅IFNβ),进入后12(T1)和24(T2)个月的结果。脑MRI在T0,T1和T2进行。在T0经历了高复发率(rr = 1.4)的30例RR患者在T1表现出年复发率(rr = 0.4)的显着改善,在T2表现出进一步的改善(rr = 0.17)(p <0.001) 。 T2时无复发的患者百分比为70%(p <0.0001)。 EDSS评分从T0时的2.6 +/- 1.23变为T2时的2.2 +/- 1.5,仅显示出改善的趋势.MRI病变负荷无明显变化,且在研究期间未记录严重不良事件。这些数据表明,CTX和IFNβ的组合可阻止活跃和恶化的MS患者的疾病进展,这表明需要使用RCT来测试该组合疗法在活跃RRMS患者或因疾病改变而经历治疗失败的患者中的疗效药物(DMD)。

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