Temple Anthony R, Benson Gordon D, Zinsenheim Joyce R, Schweinle Jo Ellen
McNeil Consumer & Specialty Pharmaceuticals, a Division of McNeil-PPC, Inc., Fort Washington, Pennsylvania 19034, USA.
Clin Ther. 2006 Feb;28(2):222-35. doi: 10.1016/j.clinthera.2006.02.004.
This study evaluated the safety of acetaminophen 4 g/d administered for up to 12 months to adult patients with osteoarthritis pain, using naproxen 750 mg/d as an active comparator.
This multicenter, multidose, single-dummy, randomized, double-blind, active-controlled, parallel-group study enrolled patients with mild to moderate osteoarthritis pain of the hip or knee. Patients received acetaminophen 4 g/d or naproxen 750 mg/d for 12 months (group 1) or 6 months (group 2). Patients in both groups had follow-up visits at months 1, 3, and 6 of treatment (or at the time of study withdrawal). Patients in group 1 also had follow-up visits at months 9 and 12 (or at the time of study withdrawal). Tolerability evaluations consisted of determinations of hepatic (aminotransferase activities) and renal (serum creatinine) function, adverse events, and physical examinations. Adverse events reported by the patient or observed by the investigator during clinical evaluation were recorded. In addition, patients were questioned at each visit regarding the occurrence of adverse events using a nonspecific question. Investigators rated the intensity of adverse events and their subjective assessment of the relationship to study medication while blinded to the treatment group. At all visits, patients completed the Western Ontario and McMaster Universities Osteoarthritis Index (WOMAC), in visual analog scale format, to assess pain, stiffness, and physical function over the previous 2 weeks. The primary efficacy end point was the mean change from baseline in the WOMAC pain subscale score at 6 months. Data from the 6- and 12-month groups were combined for analysis.
Of 581 randomized patients, the safety population included 571 patients who received > or = 1 dose of study medication. The 571 patients had a mean (SD) age of 59.3 (8.6) years, 395 (69.2%) were female, and 480 (84.1%) were white. Of 290 patients randomized to receive acetaminophen, 134 completed 3 months of treatment, 96 completed 6 months, 60 completed 9 months, and 55 completed a full 12 months. The median dose adherence ranged from 95.5% to 98.6% during the trial. The completion and adherence patterns were similar for patients receiving naproxen. Of 291 patients randomized to receive naproxen, 151 completed 3 months, 124 completed 6 months, 85 completed 9 months, and 80 completed 12 months. The median dose adherence ranged from 96.4% to 98.4% during the trial. No patient in either treatment group experienced hepatic failure, hepatic dysfunction, aminotransferase levels > or = 2x the upper limit of the reference range, renal failure, or serum creatinine levels > or = 1.5x the upper limit of the reference range. No statistically significant differences were observed between the 2 treatment groups in the proportion of patients who reported > or = 1 adverse event (206 [71.8%] acetaminophen, 209 [73.6%] naproxen) or in the proportion of patients who discontinued treatment because of adverse events (71 [24.7%] acetaminophen, 63 [22.2%] naproxen). Among adverse events considered to be drug related and reported by > or = 1% of patients, constipation and peripheral edema were reported more frequently in the naproxen group than in the acetaminophen group (9.9% vs 3.1% [P<0.002] and 3.9% vs 1.0% [P<0.033], respectively). No adverse event reported in the acetaminophen group was considered both serious and related to study medication. One subject in the naproxen group had an event that was considered serious and related to study drug: gastrointestinal bleeding. No statistically significant differences were observed between the 2 treatment groups for the primary efficacy end point.
With physician supervision, acetaminophen was found to be generally well tolerated in these patients for the treatment of osteoarthritis pain of the hip or knee for periods of up to 12 months.
本研究评估了对骨关节炎疼痛的成年患者给予每日4g对乙酰氨基酚,持续用药长达12个月的安全性,使用每日750mg萘普生作为活性对照药。
本多中心、多剂量、单盲、随机、双盲、活性对照、平行组研究纳入了髋部或膝部轻至中度骨关节炎疼痛的患者。患者接受每日4g对乙酰氨基酚或每日750mg萘普生治疗12个月(第1组)或6个月(第2组)。两组患者在治疗的第1、3和6个月(或研究退出时)进行随访。第1组患者还在第9和12个月(或研究退出时)进行随访。耐受性评估包括肝功能(转氨酶活性)和肾功能(血清肌酐)测定、不良事件及体格检查。记录患者在临床评估期间报告的或研究者观察到的不良事件。此外,每次访视时使用一个非特异性问题询问患者不良事件的发生情况。研究者在对治疗组不知情的情况下对不良事件的强度及其与研究用药关系的主观评估进行评分。在所有访视中,患者以视觉模拟量表形式完成西安大略和麦克马斯特大学骨关节炎指数(WOMAC),以评估前2周的疼痛、僵硬和身体功能。主要疗效终点是6个月时WOMAC疼痛子量表评分相对于基线的平均变化。将6个月和12个月组的数据合并进行分析。
在581例随机分组的患者中,安全人群包括571例接受了≥1剂研究用药的患者。这571例患者的平均(标准差)年龄为59.3(8.6)岁,395例(69.2%)为女性,480例(84.1%)为白人。在290例随机接受对乙酰氨基酚治疗的患者中,134例完成了3个月治疗,96例完成了6个月治疗,60例完成了9个月治疗,55例完成了完整的12个月治疗。试验期间剂量依从性中位数范围为95.5%至98.6%。接受萘普生治疗的患者的完成情况和依从模式相似。在291例随机接受萘普生治疗的患者中,151例完成了3个月治疗,124例完成了6个月治疗,85例完成了9个月治疗,80例完成了12个月治疗。试验期间剂量依从性中位数范围为96.4%至98.4%。两个治疗组中均无患者发生肝衰竭、肝功能不全、转氨酶水平≥正常参考范围上限的2倍、肾衰竭或血清肌酐水平≥正常参考范围上限的1.5倍。在报告了≥1次不良事件的患者比例(对乙酰氨基酚组206例[71.8%],萘普生组209例[73.6%])或因不良事件而停药的患者比例(对乙酰氨基酚组71例[24.7%],萘普生组63例[22.2%])方面,两个治疗组之间未观察到统计学上的显著差异。在被认为与药物相关且≥1%的患者报告的不良事件中,萘普生组便秘和外周水肿的报告频率高于对乙酰氨基酚组(分别为9.9%对3.1%[P<0.002]和3.9%对1.0%[P<0.033])。对乙酰氨基酚组报告的不良事件中没有被认为既严重又与研究用药相关的。萘普生组有1例受试者发生了被认为严重且与研究药物相关的事件:胃肠道出血。对于主要疗效终点,两个治疗组之间未观察到统计学上的显著差异。
在医生监督下,发现对乙酰氨基酚在这些患者中用于治疗髋部或膝部骨关节炎疼痛长达12个月时总体耐受性良好。
