Furst D E
Department of Medicine, University of Medicine and Dentistry of New Jersey, New Brunswick.
Drugs. 1990 Jan;39(1):19-37. doi: 10.2165/00003495-199039010-00003.
The currently available, most frequently used disease-modifying antirheumatic drugs (DMARDs) include auranofin, azathioprine, D-penicillamine, gold sodium thiomalate, hydroxychloroquine, methotrexate (amethopterin) and sulphasalazine. Controlled trials of these agents are reviewed to compare their relative efficacy and tolerability. Tender joint counts decreased with all drugs, as did joint swelling (measured as the percentage of patients with greater than or equal to 50% improvement in joint swelling). Tender joint count decreased by 8 to 57% in drug-treated patients, compared with 3 to 30% (1 study exceeded this degree of placebo response) in the placebo groups. The ratio of drug to placebo improvement usually averaged greater than 2. A 50% improvement in joint swelling occurred in between 15 and 65% of drug-treated patients. Time to onset of response varied from 6 weeks (with methotrexate) to as long as 18 months (some patients on hydroxychloroquine). The remission rate was inconsistent and unusual in controlled studies (5 to 7%), but very high in some open studies (e.g. 43%). While up to 8% of patients on DMARDs stopped therapy secondary to unsatisfactory therapeutic response (with 1 exception) up to 43% of placebo patients discontinued therapy for this reason. The ratio of dropouts for unsatisfactory therapeutic response for DMARD compared to placebo was less than 1 in 16 of 22 studies, and it was usually less than 0.5. Laboratory data examined include ESR, rheumatoid factor (RF), immunoglobulins and radiographic data. Ratios of decreases in ESR, comparing drug and placebo, were usually greater than 2. ESRs decreased from 3.6 to 27 mm/h, with gold sodium thiomalate, auranofin and methotrexate being most effective relative to placebo. RF decreased by greater than or equal to 2 tube dilutions in 15 to 53% of the DMARD groups but also decreased in up to 26% of placebo patients, with ratios of drug: placebo usually greater than 2. Immunoglobulins tended to decrease with DMARDs but the data are fragmentary. Radiographic evidence that a drug slows the rate of bony damage is strong evidence that it is a DMARD. These data, however, are not easily available because measurements of bony damage is insensitive and difficult. The best evidence of radiographic efficacy exists for gold, although the data are not uniform even here. Studies with other DMARDs suffer from lack of convincing control populations, methodological failures or small numbers, although trends exist showing that azathioprine and D-penicillamine (and perhaps sulphasalazine and methotrexate) may also slow bony deterioration. The other side of efficacy, of course, is tolerability.(ABSTRACT TRUNCATED AT 400 WORDS)
目前可用的、最常用的改变病情抗风湿药(DMARDs)包括金诺芬、硫唑嘌呤、D-青霉胺、硫代苹果酸金钠、羟氯喹、甲氨蝶呤(氨甲蝶呤)和柳氮磺胺吡啶。对这些药物的对照试验进行了综述,以比较它们的相对疗效和耐受性。所有药物治疗后压痛关节数均减少,关节肿胀情况也有所改善(以关节肿胀改善≥50%的患者百分比衡量)。药物治疗组患者的压痛关节数减少了8%至57%,而安慰剂组为3%至30%(1项研究超过了这种安慰剂反应程度)。药物与安慰剂改善效果的比值通常平均大于2。15%至65%接受药物治疗的患者关节肿胀改善了50%。起效时间从6周(甲氨蝶呤)到长达18个月(一些服用羟氯喹的患者)不等。在对照研究中缓解率不一致且较低(5%至7%),但在一些开放研究中非常高(例如43%)。使用DMARDs的患者中高达8%因治疗反应不佳而停止治疗(有1例例外),而安慰剂组因该原因停药的患者高达43%。在22项研究中的16项里,DMARDs因治疗反应不佳而停药的比例与安慰剂相比小于1/16,通常小于0.5。检查的实验室数据包括血沉(ESR)、类风湿因子(RF)、免疫球蛋白和影像学数据。比较药物和安慰剂,ESR降低的比值通常大于2。使用硫代苹果酸金钠、金诺芬和甲氨蝶呤时,ESR从3.6降至27毫米/小时,相对于安慰剂最为有效。DMARDs组中15%至53%的患者RF降低≥2个试管稀释度,但安慰剂组中高达26%的患者RF也降低,药物与安慰剂的比值通常大于2。免疫球蛋白倾向于随DMARDs降低,但数据不完整。有影像学证据表明一种药物能减缓骨损伤速度,这是其为DMARDs的有力证据。然而,这些数据不易获得,因为骨损伤测量不敏感且困难。关于金制剂的影像学疗效有最佳证据,尽管此处数据也不一致。其他DMARDs的研究存在缺乏有说服力的对照人群、方法学缺陷或样本量小的问题,不过有趋势表明硫唑嘌呤和D-青霉胺(可能还有柳氮磺胺吡啶和甲氨蝶呤)也可能减缓骨退化。当然,疗效的另一面是耐受性。(摘要截选至400字)
