Suarez-Almazor M E, Spooner C, Belseck E
Health Services Research, Veterans Affairs Medical Center, Mailbox Station 152, 2002 Holcombe Blvd, Houston, Texas, USA, 77024.
Cochrane Database Syst Rev. 2000(4):CD001460. doi: 10.1002/14651858.CD001460.
To estimate the short-term effects of D-penicillamine for the treatment of rheumatoid arthritis (RA).
We searched the Cochrane Musculoskeletal Group's trials register, the Cochrane Controlled Trials Register (issue 3, 2000) and Medline up to and including August 2000 and Embase from 1988-2000. We also carried out a handsearch of the reference lists of the trials retrieved from the electronic search.
All randomized controlled trials and controlled clinical trials comparing D-penicillamine against placebo in patients with rheumatoid arthritis.
The methodological quality of the trials was assessed independently by two reviewers (CS, EB) and checked by a third (MS) using a validated quality assessment tool (Jadad 1996). Rheumatoid arthritis outcome measures were extracted from the publications for the six-month endpoint and stratified according to D-penicillamine dosages: low (<500mg/day), moderate (500 to <1000mg/day) and high (1000 mg/day or greater). Data was abstracted by one reviewer and checked by a second (CS, MS). The pooled analysis was performed using the standardized mean difference for joint counts, pain and global assessments. The weighted mean difference was used for erythrocyte sedimentation rate (ESR). Toxicity was evaluated with pooled odds ratios for withdrawals and adverse reactions. A chi-square test was used to assess heterogeneity among trials. Fixed effects models were used throughout, since no statistical heterogeneity was found.
Six trials were identified, with 425 patients randomized to D-penacillamine and 258 to placebo. A statistically significant benefit was observed for D-penicillamine when compared to placebo for all three-dose ranges and for most outcome measures including: tender joint counts, pain, physician's global assessments and ESR. The standardized weighted mean differences between treatment and placebo in moderate doses were -0.51 [95% CI -0.88, -0.14] for tender joint counts, -0.56 (95% CI -0.87, -0.26) for pain and -0.97 (95% CI -1.25, -0.70) for global assessment. The difference for ESR was -10.6 mm/hr. Similar results were observed for the higher dose group. Total withdrawals were significantly higher in the moderate and high dosage D-penicillamine groups (OR=1.63 and 2.13 respectively), mostly due to increased adverse reactions (OR = 2.60 and 4.95 respectively), including renal and hematological abnormalities.
REVIEWER'S CONCLUSIONS: D-penicillamine appears to have a clinically and statistically significant benefit on the disease activity of patients with rheumatoid arthritis. Its efficacy appears to be similar to that of other disease modifying anti-rheumatic drugs (DMARDs), but with a significantly higher toxicity. Its effects on long-term functional status and radiological progression are not clear from this review.
评估D-青霉胺治疗类风湿关节炎(RA)的短期疗效。
我们检索了Cochrane肌肉骨骼组试验注册库、Cochrane对照试验注册库(2000年第3期)以及截至2000年8月的Medline和1988 - 2000年的Embase。我们还对电子检索获得的试验的参考文献列表进行了手工检索。
所有比较D-青霉胺与安慰剂治疗类风湿关节炎患者的随机对照试验和对照临床试验。
两名评价员(CS,EB)独立评估试验的方法学质量,第三名评价员(MS)使用经过验证的质量评估工具(Jadad,1996)进行检查。从出版物中提取类风湿关节炎结局指标,以六个月为终点,并根据D-青霉胺剂量分层:低剂量(<500mg/天)、中等剂量(500至<1000mg/天)和高剂量(1000mg/天及以上)。数据由一名评价员提取,另一名评价员(CS,MS)进行核对。采用标准化均数差值对关节计数、疼痛和整体评估进行合并分析。红细胞沉降率(ESR)采用加权均数差值。用合并比值比评估撤药和不良反应的毒性。采用卡方检验评估试验间的异质性。由于未发现统计学异质性,全程使用固定效应模型。
共识别出6项试验,425例患者随机分配至D-青霉胺组,258例患者随机分配至安慰剂组。与安慰剂相比,D-青霉胺在所有三个剂量范围以及大多数结局指标上均观察到具有统计学意义的益处,包括:压痛关节计数、疼痛、医生整体评估和ESR。中等剂量治疗组与安慰剂组在压痛关节计数方面的标准化加权均数差值为-0.51 [95%可信区间-0.88,-0.14],疼痛方面为-0.56(95%可信区间-0.87,-0.26),整体评估方面为-0.97(95%可信区间-1.25,-0.70)。ESR差值为-10.6mm/小时。高剂量组观察到类似结果。中等剂量和高剂量D-青霉胺组的总撤药率显著更高(分别为OR = 1.63和2.13),主要是由于不良反应增加(分别为OR = 2.60和4.95),包括肾脏和血液学异常。
D-青霉胺似乎对类风湿关节炎患者的疾病活动具有临床和统计学意义的益处。其疗效似乎与其他改善病情抗风湿药物(DMARDs)相似,但毒性显著更高。本综述尚不清楚其对长期功能状态和放射学进展的影响。
