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甲氨蝶呤与安慰剂治疗早期弥漫性硬皮病的随机对照试验。

A randomized, controlled trial of methotrexate versus placebo in early diffuse scleroderma.

作者信息

Pope J E, Bellamy N, Seibold J R, Baron M, Ellman M, Carette S, Smith C D, Chalmers I M, Hong P, O'Hanlon D, Kaminska E, Markland J, Sibley J, Catoggio L, Furst D E

机构信息

University of Western Ontario, London, Canada.

出版信息

Arthritis Rheum. 2001 Jun;44(6):1351-8. doi: 10.1002/1529-0131(200106)44:6<1351::AID-ART227>3.0.CO;2-I.

Abstract

OBJECTIVE

Early diffuse scleroderma (systemic sclerosis; SSc) has no proven treatment. This study was undertaken to examine the efficacy of methotrexate (MTX) in improving the skin and other disease parameters in early diffuse SSc.

METHODS

Seventy-one patients with diffuse SSc of <3 years' duration were enrolled in a multicenter, randomized, placebo-controlled, double-blind trial. Thirty-five patients were treated with MTX and 36 with placebo. Treatment was administered for 12 months. The primary outcome measures were skin score (as determined with 2 different indices) and physician global assessment.

RESULTS

At baseline, there were no statistically significant differences in skin scores, carbon monoxide diffusing capacity (DLco), physician global assessment, or other secondary outcome measurements between the 2 treatment groups. At study completion, results slightly favored the MTX group (mean +/- SEM modified Rodnan skin score 21.4+/-2.8 in the MTX group versus 26.3+/-2.1 in the placebo group [P < 0.17]; UCLA skin score 8.8+/-1.2 in the MTX group versus 11.0+/-0.9 in the placebo group [P < 0.15]; DLco in the MTX group 75.7+/-4.6 versus 61.8+/-3.4 in the placebo group [P < 0.2]). In addition, physician global assessment results favored MTX (P < 0.035), whereas patient global assessment did not differ significantly between groups. When between-group differences for changes in scores from baseline to 12 months were examined using intent-to-treat methodology, MTX appeared to have a favorable effect on skin scores (modified Rodnan score -4.3 in the MTX group versus 1.8 in the placebo group [P < 0.009]; UCLA score -1.2 in the MTX group versus 1.2 in the placebo group [P < 0.02]), but differences in the degree of change in the DLco and physician global assessment were not significant. For the UCLA skin score, these differences in results were not statistically significant after adjustment for baseline differences in sex distribution and steroid use. Dropout rates were similar in the 2 groups.

CONCLUSION

Although results of this trial demonstrated a trend in favor of MTX versus placebo in the treatment of early diffuse SSc, the between-group differences were small and the power to rule out false-negative results was only 50%. Our findings do not provide evidence that MTX is significantly effective in the treatment of early diffuse SSc.

摘要

目的

早期弥漫性硬皮病(系统性硬化症;SSc)尚无经证实有效的治疗方法。本研究旨在探讨甲氨蝶呤(MTX)改善早期弥漫性SSc皮肤及其他疾病参数的疗效。

方法

71例病程小于3年的弥漫性SSc患者纳入一项多中心、随机、安慰剂对照、双盲试验。35例患者接受MTX治疗,36例接受安慰剂治疗。治疗持续12个月。主要结局指标为皮肤评分(采用2种不同指标测定)和医生整体评估。

结果

基线时,两组在皮肤评分、一氧化碳弥散量(DLco)、医生整体评估或其他次要结局指标方面无统计学显著差异。研究结束时,结果稍有利于MTX组(MTX组改良Rodnan皮肤评分为21.4±2.8,安慰剂组为26.3±2.1 [P < 0.17];MTX组UCLA皮肤评分为8.8±1.2,安慰剂组为11.0±0.9 [P < 0.15];MTX组DLco为75.7±4.6,安慰剂组为61.8±3.4 [P < 0.2])。此外,医生整体评估结果有利于MTX(P < 0.035),而患者整体评估在两组间无显著差异。当采用意向性分析方法检查从基线到12个月评分变化的组间差异时,MTX似乎对皮肤评分有有利影响(MTX组改良Rodnan评分为 -4.3,安慰剂组为1.8 [P < 0.009];MTX组UCLA评分为 -1.2,安慰剂组为1.2 [P < 0.02]),但DLco和医生整体评估的变化程度差异不显著。对于UCLA皮肤评分,在调整性别分布和类固醇使用的基线差异后,这些结果差异无统计学意义。两组的脱落率相似。

结论

尽管本试验结果显示在治疗早期弥漫性SSc方面MTX相对于安慰剂有一定趋势,但组间差异较小,排除假阴性结果的检验效能仅为50%。我们的研究结果未提供证据表明MTX在治疗早期弥漫性SSc方面显著有效。

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