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用于急慢性疼痛的抗惊厥药物。

Anticonvulsant drugs for acute and chronic pain.

作者信息

Wiffen P, Collins S, McQuay H, Carroll D, Jadad A, Moore A

机构信息

Cochrane Pain, Palliative and Supportive Care CRG, Pain Research Unit, Churchill Hospital, Old Road, Oxford, UK, OX3 7LJ.

出版信息

Cochrane Database Syst Rev. 2000(3):CD001133. doi: 10.1002/14651858.CD001133.

Abstract

BACKGROUND

Anticonvulsant drugs have been used in the management of pain since the 1960s. The clinical impression is that they are useful for chronic neuropathic pain, especially when the pain is lancinating or burning.

OBJECTIVES

To evaluate the analgesic effectiveness and adverse effects of anticonvulsant drugs for pain management in clinical practice and to identify a clinical research agenda. Migraine and headache studies are excluded in this revision.

SEARCH STRATEGY

Randomised trials of anticonvulsants in acute, chronic or cancer pain were identified by Medline (1966-1999), Embase (1994-1999), SIGLE (1980-1999) and the Cochrane Controlled Trials Register (CENTRAL/CCTR) (Cochrane Library Issue 3, 1999). In addition, 40 medical journals were hand searched. Additional reports were identified from the reference list of the retrieved papers, and by contacting investigators. Date of most recent search: September 1999.

SELECTION CRITERIA

Randomised trials reporting the analgesic effects of anticonvulsant drugs in patients, with subjective pain assessment as either the primary or a secondary outcome.

DATA COLLECTION AND ANALYSIS

Data were extracted by two independent reviewers, and trials were quality scored. Numbers-needed-to-treat (NNTs) were calculated from dichotomous data for effectiveness, adverse effects and drug-related study withdrawal, for individual studies and for pooled data.

MAIN RESULTS

Twenty-three trials of six anticonvulsants were considered eligible (1,074 patients). The only placebo-controlled study in acute pain found no analgesic effect of sodium valproate. Three placebo-controlled studies of carbamazepine in trigeminal neuralgia had a combined NNT (95% confidence interval (CI)) for effectiveness of 2.5 (CI 2.0-3.4). A single placebo-controlled trial of gabapentin in post-herpetic neuralgia had an NNT of 3.2 (CI 2.4-5.0). For diabetic neuropathy NNTs for effectiveness were as follows: (one RCT for each drug) carbamazepine 2.3 (CI 1.6-3.8), gabapentin 3.8 (CI 2.4-8.7) and phenytoin 2.1 (CI 1.5-3.6). Numbers-needed-to-harm (NNHs) were calculated where possible by combining studies for each drug entity irrespective of the condition treated. The results were, for minor harm, carbamazepine 3.7 (CI 2.4-7.8), gabapentin 2.5 (CI 2.0-3.2), phenytoin 3.2 (CI 2.1-6.3). NNHs for major harm were not statistically significant for any drug compared with placebo. Phenytoin had no effect in irritable bowel syndrome, and carbamazepine little effect in post-stroke pain. Clonazepam was effective in one study of temporomandibular joint dysfunction.

REVIEWER'S CONCLUSIONS: Although anticonvulsants are used widely in chronic pain surprisingly few trials show analgesic effectiveness. No trial compared different anticonvulsants. Only one studied considered cancer pain. There is no evidence that anticonvulsants are effective for acute pain. In chronic pain syndromes other than trigeminal neuralgia, anticonvulsants should be withheld until other interventions have been tried. While gabapentin is increasingly being used for neuropathic pain the evidence would suggest that it is not superior to carbamazepine.

摘要

背景

自20世纪60年代以来,抗惊厥药物一直用于疼痛管理。临床印象是,它们对慢性神经性疼痛有用,尤其是当疼痛呈刺痛或灼痛时。

目的

评估抗惊厥药物在临床实践中用于疼痛管理的镇痛效果和不良反应,并确定临床研究议程。本次修订排除偏头痛和头痛研究。

检索策略

通过医学索引数据库(1966 - 1999年)、荷兰医学文摘数据库(1994 - 1999年)、灰色文献数据库(1980 - 1999年)和考克兰对照试验注册库(CENTRAL/CCTR)(考克兰图书馆1999年第3期)确定抗惊厥药物治疗急性、慢性或癌痛的随机试验。此外,还手工检索了40种医学期刊。从检索到的论文参考文献列表以及与研究者联系中确定了其他报告。最近一次检索日期:1999年9月。

选择标准

报告抗惊厥药物对患者镇痛效果的随机试验,以主观疼痛评估作为主要或次要结局。

数据收集与分析

由两名独立审阅者提取数据,并对试验进行质量评分。根据二分数据计算个体研究和汇总数据的治疗所需人数(NNT),用于评估有效性、不良反应和与药物相关的研究撤药情况。

主要结果

六项抗惊厥药物的23项试验被认为符合条件(1074例患者)。唯一一项急性疼痛的安慰剂对照研究未发现丙戊酸钠有镇痛效果。三项卡马西平治疗三叉神经痛的安慰剂对照研究的合并NNT(95%置信区间(CI))为2.5(CI 2.0 - 3.4)。一项加巴喷丁治疗带状疱疹后神经痛的安慰剂对照试验的NNT为3.2(CI 2.4 - 5.0)。糖尿病性神经病变有效性的NNT如下:(每种药物一项随机对照试验)卡马西平2.3(CI 1.6 - 3.8),加巴喷丁3.8(CI 2.4 - 8.7),苯妥英2.1(CI 1.5 - 3.6)。在可能的情况下,通过合并每种药物实体的研究计算伤害所需人数(NNH),无论治疗的疾病如何。结果显示,轻微伤害方面,卡马西平3.7(CI 2.4 - 7.8),加巴喷丁2.5(CI 2.0 - 3.2),苯妥英3.2(CI 2.1 - 6.3)。与安慰剂相比,任何药物严重伤害的NNH均无统计学意义。苯妥英对肠易激综合征无效,卡马西平对中风后疼痛效果甚微。氯硝西泮在一项颞下颌关节功能障碍研究中有效。

审阅者结论

尽管抗惊厥药物在慢性疼痛中广泛使用,但令人惊讶的是,很少有试验显示出镇痛效果。没有试验比较不同的抗惊厥药物。只有一项研究考虑了癌痛。没有证据表明抗惊厥药物对急性疼痛有效。在三叉神经痛以外的慢性疼痛综合征中,在尝试其他干预措施之前应停用抗惊厥药物。虽然加巴喷丁越来越多地用于神经性疼痛,但证据表明它并不优于卡马西平。

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