Once weekly interferon beta for multiple sclerosis is superseded by higher and more frequent dosing.

L D Blumhardt
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Abstract

Therapy with interferon (IFN) beta can significantly alter the disease course in relapsing-remitting multiple sclerosis. Evidence indicates that the efficacy of this agent is related to treatment regimen (dose, route and dose frequency). A higher total weekly dose administered several times a week provides greater clinical benefit than a lower dose given once weekly (q.w.). This dose- and dose frequency-dependency of the efficacy of IFN beta has been clearly demonstrated in three recent head-to-head studies, as well as in other major clinical trials, and pharmacodynamic, pharmacokinetic and pre-clinical studies. The use of a q.w. dose regimen of IFN beta is likely to have a negative impact on patients in both the short and long-term because it allows additional accumulation of irreversible tissue damage in the central nervous system. Patients should receive the optimal, more rapid benefits from higher and more frequent doses of IFN beta, administered as early as possible after diagnosis.

对于多发性硬化症,每周一次的干扰素β被更高、更频繁的剂量所取代。
干扰素治疗可以显著改变复发缓解型多发性硬化症的病程。有证据表明,该药物的疗效与治疗方案(剂量、途径和剂量频率)有关。较高的每周总剂量每周给药几次比较低的每周给药一次提供更大的临床效益。最近的三项头对头研究以及其他主要临床试验、药效学、药代动力学和临床前研究清楚地证明了IFN - β的剂量和剂量频率依赖性。使用q.w剂量的IFN β可能在短期和长期对患者产生负面影响,因为它允许中枢神经系统中不可逆组织损伤的额外积累。患者应在诊断后尽早给予更高和更频繁剂量的干扰素β,从而获得最佳的、更快的益处。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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