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曲马多/右旋酮洛芬(TRAM/DKP)与曲马多/对乙酰氨基酚在中重度急性疼痛中的比较:一项在第三磨牙阻生拔牙疼痛模型中进行的随机、双盲、安慰剂和阳性药物对照、平行组试验(DAVID 研究)的结果。

Tramadol/dexketoprofen (TRAM/DKP) compared with tramadol/paracetamol in moderate to severe acute pain: results of a randomised, double-blind, placebo and active-controlled, parallel group trial in the impacted third molar extraction pain model (DAVID study).

机构信息

Department of Oral and Maxillofacial Surgery, Bellvitge Biomedical Research Institute (IDIBELL), School of Dentistry, Hospital Duran i Reynals, Barcelona, Spain.

Analgesics & Pain Research (APR) Ltd, Beckenham, UK.

出版信息

BMJ Open. 2019 Feb 19;9(2):e023715. doi: 10.1136/bmjopen-2018-023715.

Abstract

OBJECTIVES

To compare efficacy/safety of oral tramadol 75 mg/dexketoprofen 25 mg (TRAM/DKP) and TRAM 75 mg/paracetamol 650 mg (TRAM/paracetamol) in moderate to severe pain following surgical removal of impacted lower third molar.

DESIGN

Multicentre, randomised, double-blind, placebo-controlled, phase IIIb study.

PARTICIPANTS

Healthy adult patients scheduled for surgical extraction of at least one fully/partially impacted lower third molar requiring bone manipulation. 654 patients were randomised and 653 were eligible for analysis.

INTERVENTIONS

Surgery was performed under local anaesthetic. No sedation was permitted. Patients rated pain intensity (PI) using an 11-Numerical Rating Scale (NRS) (0 no pain; 10 worst pain). Participants experiencing moderate/severe pain (≥4) within 4 hours of surgery were randomised (2:2:1 ratio) to a single oral dose of TRAM/DKP 75/25 mg, TRAM/paracetamol 75/650 mg or placebo.

MAIN OUTCOME MEASURES

Efficacy was based patients' electronic diaries. Analgesia and pain were recorded as follows: pain relief (PAR) on a 5-point Verbal Rating Scale (0='no relief', 1='a little (perceptible) relief', 2='some (meaningful) relief', 3='lot of relief', 4='complete relief') at the predefined postdose time points t15 min, t30 min, t1 hour, t1.5 hour, t2 hour, t4 hour, t6 hour and t8 hour and PI on the 11-point NRS at t0 and at the same predefined postdose time points. Onset of analgesia documented using double stopwatch method over a 2-hour period. Primary endpoint was total pain relief over 6 hours (TOTPAR6). Rescue medication was available during the treatment period.

RESULTS

TRAM/DKP was superior to TRAM/paracetamol and placebo at the primary endpoint TOTPAR6 (p<0.0001). Mean (SD) TOTPAR6 in the TRAM/DKP group was 13 (6.97), while those in the active control and placebo groups were 9.2 (7.65) and 1.9 (3.89), respectively. Superiority of TRAM/DKP over active comparator and placebo was observed at all secondary endpoints. Incidence of adverse events was comparable between active groups.

CONCLUSIONS

TRAM/DKP (75/25 mg) is effective and superior to TRAM/paracetamol (75/650 mg) in relieving moderate to severe acute pain following surgical removal of impacted lower third molar, with a faster onset of action, greater and durable analgesia, together with a favourable safety profile.

TRIAL REGISTRATION NUMBER

EudraCT 2015-004152-22 and NCT02777970.

摘要

目的

比较口服曲马多 75mg/右旋酮洛芬 25mg(TRAM/DKP)与曲马多 75mg/对乙酰氨基酚 650mg(TRAM/对乙酰氨基酚)在第三磨牙完全/部分阻生手术后中重度疼痛的疗效/安全性。

设计

多中心、随机、双盲、安慰剂对照、IIIb 期研究。

参与者

计划接受至少一颗完全/部分阻生的第三磨牙手术切除的健康成年患者,需要进行骨操作。654 名患者被随机分组,653 名患者符合分析条件。

干预措施

手术在局部麻醉下进行。不允许镇静。患者使用 11 点数字评分量表(NRS)(0 无疼痛;10 最痛)来评估疼痛强度(PI)。术后 4 小时内出现中度/重度疼痛(≥4)的患者(2:2:1 比例)随机接受单次口服 TRAM/DKP 75/25mg、TRAM/对乙酰氨基酚 75/650mg 或安慰剂。

主要观察指标

根据患者的电子日记评估疗效。镇痛和疼痛记录如下:在预定的给药后时间点 t15min、t30min、t1 小时、t1.5 小时、t2 小时、t4 小时、t6 小时和 t8 小时,使用 5 分制口头评分量表(0=无缓解,1=略有缓解(可察觉),2=有一定缓解,3=缓解明显,4=完全缓解)评估疼痛缓解(PAR),以及在 t0 和相同预定的给药后时间点使用 11 点 NRS 评估 PI。镇痛起效时间通过双秒表法记录 2 小时。主要终点是 6 小时内的总疼痛缓解(TOTPAR6)。在治疗期间可使用解救药物。

结果

TRAM/DKP 在主要终点 TOTPAR6 方面优于 TRAM/对乙酰氨基酚和安慰剂(p<0.0001)。TRAM/DKP 组的平均(SD)TOTPAR6 为 13(6.97),而活性对照组和安慰剂组分别为 9.2(7.65)和 1.9(3.89)。TRAM/DKP 在所有次要终点均优于活性对照组和安慰剂。活性组之间不良反应的发生率相似。

结论

TRAM/DKP(75/25mg)在缓解第三磨牙完全/部分阻生手术后的中重度急性疼痛方面有效且优于 TRAM/对乙酰氨基酚(75/650mg),起效更快,镇痛效果更强且持久,安全性良好。

试验注册

EudraCT 2015-004152-22 和 NCT02777970。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/52c1/6377526/097cd56f0ceb/bmjopen-2018-023715f01.jpg

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