Department of Interdisciplinary Intensive Care, Jagiellonian University Collegium Medicum, Krakow, Poland.
University Hospital, Krakow, Poland.
Cochrane Database Syst Rev. 2022 May 19;5(5):CD010967. doi: 10.1002/14651858.CD010967.pub3.
Clonidine is a presynaptic alpha-2-adrenergic receptor agonist that has been used for many years to treat hypertension and other conditions, including chronic pain. Adverse events associated with systemic use of the drug have limited its application. Topical use of drugs has been gaining interest since the beginning of the century, as it may limit adverse events without loss of analgesic efficacy. Topical clonidine (TC) formulations have been investigated for almost 20 years in clinical trials. This is an update of the original Cochrane Review published in Issue 8, 2015.
The objective of this review was to assess the analgesic efficacy and safety of TC compared with placebo or other drugs in adults aged 18 years or above with chronic neuropathic pain.
For this update we searched the Cochrane Register of Studies Online (CRSO), MEDLINE (Ovid), and Embase (Ovid) databases, and reference lists of retrieved papers and trial registries. We also contacted experts in the field. The most recent search was performed on 27 October 2021.
We included randomised, double-blind studies of at least two weeks' duration comparing TC versus placebo or other active treatment in adults with chronic neuropathic pain.
Two review authors independently screened references for eligibility, extracted data, and assessed risk of bias. Any discrepancies were resolved by discussion or by consulting a third review author if necessary. Where required, we contacted trial authors to request additional information. We presented pooled estimates for dichotomous outcomes as risk ratios (RRs) with 95% confidence intervals (CIs), and continuous outcomes as mean differences (MDs) with P values. We used Review Manager Web software to perform the meta-analyses. We used a fixed-effect model if we considered heterogeneity as not important; otherwise, we used a random-effects model. The review primary outcomes were: participant-reported pain relief of 50% or greater; participant-reported pain relief of 30% or greater; much or very much improved on Patient Global Impression of Change scale (PGIC); and very much improved on PGIC. Secondary outcomes included withdrawals due to adverse events; participants experiencing at least one adverse event; and withdrawals due to lack of efficacy. All outcomes were measured at the longest follow-up period. We assessed the certainty of evidence using GRADE and created two summary of findings tables.
We included four studies in the review (two new in this update), with a total of 743 participants with painful diabetic neuropathy (PDN). TC (0.1% or 0.2%) was applied in gel form to the painful area two to three times daily. The double-blind treatment phase of three studies lasted 8 weeks to 85 days and compared TC versus placebo. In the fourth study, the double-blind treatment phase lasted 12 weeks and compared TC versus topical capsaicin. We assessed the studies as at unclear or high risk of bias for most domains; all studies were at unclear risk of bias for allocation concealment and blinding of outcome assessment; one study was at high risk of bias for blinding of participants and personnel; two studies were at high risk of attrition bias; and three studies were at high risk of bias due to notable funding concerns. We judged the certainty of evidence (GRADE) to be moderate to very low, downgrading for study limitations, imprecision of results, and publication bias. TC compared to placebo There was no evidence of a difference in number of participants with participant-reported pain relief of 50% or greater during longest follow-up period (12 weeks) between groups (risk ratio (RR) 1.21, 95% confidence interval (CI) 0.78 to 1.86; 179 participants; 1 study; low certainty evidence). However, the number of participants with participant-reported pain relief of 30% or greater during longest follow-up period (8 to 12 weeks) was higher in the TC group compared with placebo (RR 1.35, 95% CI 1.03 to 1.77; 344 participants; 2 studies, very low certainty evidence). The number needed to treat for an additional beneficial outcome (NNTB) for this comparison was 8.33 (95% CI 4.3 to 50.0). Also, there was no evidence of a difference between groups for the outcomes much or very much improved on the PGIC during longest follow-up period (12 weeks) or very much improved on PGIC during the longest follow-up period (12 weeks) (RR 1.06, 95% CI 0.76 to 1.49 and RR 1.82, 95% CI 0.89 to 3.72, respectively; 179 participants; 1 study; low certainty evidence). We observed no evidence of a difference between groups in withdrawals due to adverse events and withdrawals due to lack of efficacy during the longest follow-up period (12 weeks) (RR 0.34, 95% CI 0.04 to 3.18 and RR 1.01, 95% CI 0.06 to 15.92, respectively; 179 participants; 1 study; low certainty evidence) and participants experiencing at least one adverse event during longest follow-up period (12 weeks) (RR 0.65, 95% CI 0.14 to 3.05; 344 participants; 2 studies; low certainty evidence). TC compared to active comparator There was no evidence of a difference in the number of participants with participant-reported pain relief of 50% or greater during longest follow-up period (12 weeks) between groups (RR 1.41, 95% CI 0.99 to 2.0; 139 participants; 1 study; low certainty evidence). Other outcomes were not reported.
AUTHORS' CONCLUSIONS: This is an update of a review published in 2015, for which our conclusions remain unchanged. Topical clonidine may provide some benefit to adults with painful diabetic neuropathy; however, the evidence is very uncertain. Additional trials are needed to assess TC in other neuropathic pain conditions and to determine whether it is possible to predict who or which groups of people will benefit from TC.
可乐定是一种具有多年历史的用于治疗高血压和其他疾病(包括慢性疼痛)的突触前α-2 肾上腺素能受体激动剂。全身性使用该药物引起的不良反应限制了其应用。自本世纪初以来,人们对药物的局部应用产生了兴趣,因为它可能在不降低镇痛效果的情况下限制不良反应。在临床试验中,已经对局部用可乐定(TC)制剂进行了近 20 年的研究。这是对 2015 年第 8 期原始 Cochrane 综述的更新。
本综述的目的是评估与安慰剂或其他药物相比,TC 在年龄在 18 岁及以上的慢性神经性疼痛的成年人中的镇痛疗效和安全性。
本次更新,我们检索了 Cochrane 对照试验注册库(CRSO)、MEDLINE(Ovid)和 Embase(Ovid)数据库,以及检索文献的参考文献列表和试验注册处。我们还联系了该领域的专家。最近一次检索是在 2021 年 10 月 27 日进行的。
我们纳入了至少持续两周的随机、双盲研究,比较了 TC 与安慰剂或其他活性治疗在慢性神经性疼痛的成年人中的疗效。
两名综述作者独立筛选参考文献的纳入性、提取数据,并评估偏倚风险。如有分歧,通过讨论或必要时咨询第三名综述作者解决。如有需要,我们联系了试验作者以请求额外的信息。我们以风险比(RR)和 95%置信区间(CI)的形式呈现二分类结局的汇总估计值,以均值差(MD)和 P 值的形式呈现连续性结局的汇总估计值。我们使用 Review Manager Web 软件进行荟萃分析。如果我们认为异质性不重要,则使用固定效应模型;否则,使用随机效应模型。该综述的主要结局包括:参与者报告的疼痛缓解 50%或以上;参与者报告的疼痛缓解 30%或以上;患者整体印象变化量表(PGIC)上的“大有改善”或“非常改善”;PGIC 上的“非常改善”。次要结局包括:因不良事件而退出;至少有一次不良事件的参与者;以及因缺乏疗效而退出。所有结局都在最长随访期间进行测量。我们使用 GRADE 评估证据的确定性,并创建了两个总结结局表格。
我们纳入了四项研究(两项为本次更新中的新研究),共有 743 名患有痛性糖尿病性神经病变(PDN)的参与者。TC(0.1%或 0.2%)以凝胶形式涂于疼痛区域,每日两次至三次。三项研究的双盲治疗阶段持续 8 周至 85 天,比较 TC 与安慰剂;第四项研究的双盲治疗阶段持续 12 周,比较 TC 与局部用辣椒素。我们评估了大多数领域的研究,认为其具有高偏倚风险或高度不确定;所有研究在分配隐藏和结局评估的盲法方面都具有高度不确定的偏倚风险;一项研究在参与者和人员的盲法方面具有高度偏倚风险;两项研究在失访偏倚方面具有高度偏倚风险;三项研究由于明显的资金问题而具有高度偏倚风险。我们判断证据的确定性(GRADE)为中度至非常低,降级的原因包括研究局限性、结果不精确性和发表偏倚。TC 与安慰剂相比,在最长随访期间(12 周),报告的疼痛缓解 50%或以上的参与者比例无差异(风险比(RR)1.21,95%置信区间(CI)0.78 至 1.86;179 名参与者;1 项研究;低确定性证据)。然而,在 TC 组中,报告的疼痛缓解 30%或以上的参与者比例在最长随访期间(8 至 12 周)更高(RR 1.35,95%CI 1.03 至 1.77;344 名参与者;2 项研究,低确定性证据)。在这项比较中,需要治疗的人数(NNTB)为 8.33(95%CI 4.3 至 50.0)。此外,在最长随访期间(12 周),PGIC 上的“大有改善”或“非常改善”或在最长随访期间(12 周)PGIC 上的“非常改善”方面,两组之间无差异(RR 1.06,95%CI 0.76 至 1.49 和 RR 1.82,95%CI 0.89 至 3.72;179 名参与者;1 项研究;低确定性证据)。我们在最长随访期间(12 周)因不良事件和缺乏疗效而退出的参与者之间没有观察到差异(RR 0.34,95%CI 0.04 至 3.18 和 RR 1.01,95%CI 0.06 至 15.92;179 名参与者;1 项研究;低确定性证据)和至少经历过一次不良事件的参与者(RR 0.65,95%CI 0.14 至 3.05;344 名参与者;2 项研究;低确定性证据)。TC 与活性对照相比,在最长随访期间(12 周),报告的疼痛缓解 50%或以上的参与者比例无差异(RR 1.41,95%CI 0.99 至 2.0;139 名参与者;1 项研究;低确定性证据)。其他结局未报告。
这是对 2015 年发表的一项综述的更新,我们的结论保持不变。局部用可乐定可能对患有痛性糖尿病性神经病变的成年人有一定益处;然而,证据非常不确定。需要进一步的试验来评估 TC 在其他神经性疼痛疾病中的疗效,并确定是否有可能预测哪些人或哪些人群将从 TC 中受益。
