Cacione Daniel G, Baptista-Silva Jose C C, Macedo Cristiane R
Department of Surgery, UNIFESP - Escola Paulista de Medicina, Rua Borges Lagoa, 564 cj 124, Vila Clementino, São Paulo, Brazil, 04038000.
Cochrane Database Syst Rev. 2016 Feb 1;2:CD011033. doi: 10.1002/14651858.CD011033.pub2.
Buerger's disease (thromboangiitis obliterans) is a non-atherosclerotic, segmental inflammatory pathology that most commonly affects the small and medium sized arteries, veins, and nerves in the upper and lower extremities. The etiology is unknown, but involves hereditary susceptibility, tobacco exposure, immune and coagulation responses. In many cases, there is no possibility of revascularization to improve the condition. Pharmacological treatment is an option for patients with severe complications, such as ischaemic ulcers or rest pain.
To assess the effectiveness of any pharmacological agent (intravenous or oral) compared with placebo or any other pharmacological agent in patients with Buerger's disease.
The Cochrane Vascular Trials Search Co-ordinator searched their Specialised Register (last searched in April 2015) and the Cochrane Register of Studies (Issue 3, 2015). The review authors searched trial registers and the European grey literature; screened reference lists of relevant studies, and contacted study authors and major pharmaceutical companies.
Randomised controlled trials (RCTs) involving pharmacological agents used in the treatment of Buerger's disease.
Two review authors, independently assessed the studies, extracted data and performed data analysis.
Five randomised controlled trials (total 602 participants) compared prostacyclin analogue with placebo, aspirin, or a prostaglandin analogue, and folic acid with placebo. No studies assessed other pharmacological agents such as cilostazol, clopidogrel and pentoxifylline or compared oral versus intravenous prostanoid.Compared with aspirin, intravenous prostacyclin analogue iloprost improved ulcer healing (risk ratio (RR) 2.65; 95% confidence interval (CI) 1.15 to 6.11; 98 participants; one study; moderate quality evidence), and helped to eradicate rest pain after 28 days (RR 2.28; 95% CI 1.48 to 3.52; 133 participants; one study; moderate quality evidence), although amputation rates were similar six months after treatment (RR 0.32; 95% CI 0.09 to 1.15; 95 participants; one study; moderate quality evidence). When comparing prostacyclin (iloprost and clinprost) with prostaglandin (alprostadil) analogues, ulcer healing was similar (RR 1.13; 95% CI 0.76 to 1.69; 89 participants; two studies; I² = 0%; very low quality evidence), as was the eradication of rest pain after 28 days (RR 1.57; 95% CI 0.72 to 3.44; 38 participants; one study; low quality evidence), while amputation rates were not measured. Compared with placebo, the effects of oral prostacyclin analogue iloprost were similar for: healing ischaemic ulcers (iloprost 200 mcg: RR 1.11; 95% CI 0.54 to 2.29; 133 participants; one study; moderate quality evidence, and iloprost 400 mcg: RR 0.90; 95% CI 0.42 to 1.93; 135 participants; one study; moderate quality evidence), eradication of rest pain after eight weeks (iloprost 200 mcg: RR 1.14; 95% CI 0.79 to 1.63; 207 participants; one study; moderate quality evidence, and iloprost 400 mcg: RR 1.11; 95% CI 0.77 to 1.59; 201 participants; one study; moderate quality evidence), and amputation rates after six months (iloprost 200 mcg: RR 0.54; 95% CI 0.19 to 1.56; 209 participants; one study, and iloprost 400 mcg: RR 0.42; 95% CI 0.13 to 1.31; 213 participants; one study). When comparing folic acid with placebo in patients with Buerger's disease and hyperhomocysteinaemia, pain scores were similar, there were no new cases of amputation in either group, and ulcer healing was not assessed (very low quality evidence).Treatment side effects such as headaches, flushing or nausea were not associated with treatment interruptions or more serious consequences. Outcomes such as amputation-free survival, walking distance or pain-free walking distance, and ankle brachial index were not assessed by any study.Overall, the quality of the evidence was very low to moderate, with few studies, small numbers of participants, variation in severity of disease of participants between studies and missing information regarding for example baseline tobacco exposure.
AUTHORS' CONCLUSIONS: Moderate quality evidence suggests that intravenous iloprost (prostacyclin analogue) is more effective than aspirin for eradicating rest pain and healing ischaemic ulcers in Buerger's disease, but oral iloprost is not more effective than placebo. Verylow and low quality evidence suggests there is no difference between prostacyclin (iloprost and clinprost) and the prostaglandin analogue alprostadil for healing ulcers and relieving pain respectively in severe Buerger's disease. Very-low quality evidence suggests there is no difference in pain scores and amputation rates between folic acid and placebo, in people with Buerger's disease and hyperhomocysteinaemia. High quality trials assessing the effectiveness of pharmacological agents (intravenous or oral) in people with Buerger's disease are needed.
血栓闭塞性脉管炎是一种非动脉粥样硬化性、节段性炎症性病变,最常累及上下肢的中小动脉、静脉和神经。病因不明,但涉及遗传易感性、烟草暴露、免疫和凝血反应。在许多情况下,无法进行血管重建来改善病情。药物治疗是患有严重并发症(如缺血性溃疡或静息痛)患者的一种选择。
评估任何药物(静脉或口服)与安慰剂或任何其他药物相比,在血栓闭塞性脉管炎患者中的疗效。
Cochrane血管试验搜索协调员检索了他们的专业注册库(最后检索时间为2015年4月)和Cochrane研究注册库(2015年第3期)。综述作者检索了试验注册库和欧洲灰色文献;筛选了相关研究的参考文献列表,并联系了研究作者和主要制药公司。
涉及用于治疗血栓闭塞性脉管炎的药物的随机对照试验(RCT)。
两位综述作者独立评估研究、提取数据并进行数据分析。
五项随机对照试验(共602名参与者)比较了前列环素类似物与安慰剂、阿司匹林或前列腺素类似物,以及叶酸与安慰剂。没有研究评估其他药物,如西洛他唑、氯吡格雷和己酮可可碱,也没有比较口服与静脉注射前列腺素。与阿司匹林相比,静脉注射前列环素类似物伊洛前列素可改善溃疡愈合(风险比(RR)2.65;95%置信区间(CI)1.15至6.11;98名参与者;一项研究;中等质量证据),并有助于在28天后消除静息痛(RR 2.28;95%CI 1.48至3.52;133名参与者;一项研究;中等质量证据),尽管治疗六个月后的截肢率相似(RR 0.32;95%CI 0.09至1.15;95名参与者;一项研究;中等质量证据)。当比较前列环素(伊洛前列素和克林前列素)与前列腺素(前列地尔)类似物时,溃疡愈合情况相似(RR 1.13;95%CI 0.76至1.69;89名参与者;两项研究;I² = 0%;极低质量证据),28天后消除静息痛的情况也相似(RR 1.57;95%CI 0.72至3.44;38名参与者;一项研究;低质量证据),而未测量截肢率。与安慰剂相比,口服前列环素类似物伊洛前列素在以下方面效果相似:愈合缺血性溃疡(伊洛前列素200 mcg:RR 1.11;95%CI 0.54至2.29;133名参与者;一项研究;中等质量证据,伊洛前列素400 mcg:RR 0.90;95%CI 0.42至1.93;135名参与者;一项研究;中等质量证据),八周后消除静息痛(伊洛前列素200 mcg:RR 1.14;9%CI 0.79至1.63;207名参与者;一项研究;中等质量证据,伊洛前列素400 mcg:RR 1.11;95%CI 0.77至1.59;201名参与者;一项研究;中等质量证据),以及六个月后的截肢率(伊洛前列素200 mcg:RR 0.54;95%CI 0.19至1.56;209名参与者;一项研究,伊洛前列素400 mcg:RR 0.42;95%CI 0.13至1.31;213名参与者;一项研究)。在血栓闭塞性脉管炎和高同型半胱氨酸血症患者中比较叶酸与安慰剂时,疼痛评分相似,两组均无新的截肢病例,且未评估溃疡愈合情况(极低质量证据)。治疗副作用如头痛、潮红或恶心与治疗中断或更严重后果无关。任何研究均未评估无截肢生存、步行距离或无痛步行距离以及踝臂指数等结局。总体而言,证据质量极低至中等,研究较少,参与者数量少,各研究中参与者疾病严重程度存在差异,且缺少例如基线烟草暴露等信息。
中等质量证据表明,静脉注射伊洛前列素(前列环素类似物)在消除血栓闭塞性脉管炎患者的静息痛和愈合缺血性溃疡方面比阿司匹林更有效,但口服伊洛前列素并不比安慰剂更有效。极低和低质量证据表明,在严重血栓闭塞性脉管炎中,前列环素(伊洛前列素和克林前列素)与前列腺素类似物前列地尔在愈合溃疡和缓解疼痛方面分别无差异。极低质量证据表明,在血栓闭塞性脉管炎和高同型半胱氨酸血症患者中,叶酸与安慰剂在疼痛评分和截肢率方面无差异。需要高质量试验来评估药物(静脉或口服)在血栓闭塞性脉管炎患者中的疗效。
