Li D K, Paty D W
Department of Radiology, UBC Hospital, Vancouver, BC, Canada.
Ann Neurol. 1999 Aug;46(2):197-206. doi: 10.1002/1531-8249(199908)46:2<197::aid-ana9>3.0.co;2-p.
The PRISMS (Prevention of Relapses and Disability by Interferon-beta1a Subcutaneously in Multiple Sclerosis) trial was a double-blind, randomized, multicenter, phase III, placebo-controlled study of interferon-beta1a in 560 patients from 22 centers in 9 countries with clinically definite or laboratory-supported relapsing-remitting multiple sclerosis. The patients were randomized to receive recombinant interferon-beta1a (Rebif), 22 microg (6 mIU), 44 microg (12 mIU), or placebo, given subcutaneously, three times weekly for 2 years. All patients underwent biannual proton density/T2-weighted magnetic resonance imaging scans to determine the overall magnetic resonance imaging disease activity and burden of disease, and a cohort of 205 patients had 11 initial monthly proton density/T2-weighted and gadolinium-enhanced/T1-weighted magnetic resonance imaging scans. Over the 2 years, the placebo group showed a progressive median increase in burden of disease of 10.9%, whereas the 22-microg group and 44-microg group showed median decreases of 1.2% and 3.8%, respectively. The number of T2 active lesions and percentage of scans showing T2 activity on the biannual scans were also significantly reduced in both treatment groups compared with placebo, with a clear dose-effect favoring the 44-microg dose over the 22-microg dose. In the subgroup undergoing initial monthly scanning, this reduction in activity became statistically significant 2 months after the start of treatment. These results provide strong, objective evidence to support the positive clinical results of reduction in relapses and delay in disease progression. In addition, they also demonstrate a significant dosage effect, favoring the 44-microg dose.
PRISMS(皮下注射β-干扰素1a预防多发性硬化症复发和残疾)试验是一项双盲、随机、多中心、III期、安慰剂对照研究,研究对象为来自9个国家22个中心的560例临床确诊或实验室支持的复发缓解型多发性硬化症患者。患者被随机分为皮下注射重组β-干扰素1a(Rebif)22微克(6百万国际单位)、44微克(12百万国际单位)或安慰剂组,每周3次,共2年。所有患者每半年接受一次质子密度/T2加权磁共振成像扫描,以确定总体磁共振成像疾病活动度和疾病负担,205例患者最初每月进行11次质子密度/T2加权及钆增强/T1加权磁共振成像扫描。在2年期间,安慰剂组疾病负担中位数渐进性增加10.9%,而22微克组和44微克组中位数分别下降1.2%和3.8%。与安慰剂相比,两个治疗组半年期扫描中T2活跃病灶数量及显示T2活动的扫描百分比也显著降低,有明确的剂量效应,44微克剂量优于22微克剂量。在最初每月进行扫描的亚组中,治疗开始2个月后活动度降低具有统计学意义。这些结果提供了有力的客观证据,支持减少复发和延缓疾病进展的积极临床结果。此外,它们还显示出显著的剂量效应,支持44微克剂量。