Estcourt Lise J, Desborough Michael, Brunskill Susan J, Doree Carolyn, Hopewell Sally, Murphy Michael F, Stanworth Simon J
Haematology/Transfusion Medicine, NHS Blood and Transplant, Level 2, John Radcliffe Hospital, Headington, Oxford, UK, OX3 9BQ.
Cochrane Database Syst Rev. 2016 Mar 15;3(3):CD009733. doi: 10.1002/14651858.CD009733.pub3.
People with haematological disorders are frequently at risk of severe or life-threatening bleeding as a result of thrombocytopenia (reduced platelet count). This is despite the routine use of prophylactic platelet transfusions to prevent bleeding once the platelet count falls below a certain threshold. Platelet transfusions are not without risk and adverse events may be life-threatening. A possible adjunct to prophylactic platelet transfusions is the use of antifibrinolytics, specifically the lysine analogues tranexamic acid (TXA) and epsilon aminocaproic acid (EACA). This is an update of a Cochrane review first published in 2013.
To determine the efficacy and safety of antifibrinolytics (lysine analogues) in preventing bleeding in people with haematological disorders.
We searched for randomised controlled trials (RCTs) in the Cochrane Central Register of Controlled Trials (The Cochrane Library 2016, Issue 3), MEDLINE (from 1946), Embase (from 1974), CINAHL (from 1937), the Transfusion Evidence Library (from 1950) and ongoing trial databases to 07 March 2016.
We included RCTs involving participants with haematological disorders, who would routinely require prophylactic platelet transfusions to prevent bleeding. We only included trials involving the use of the lysine analogues TXA and EACA.
Two review authors independently screened all electronically-derived citations and abstracts of papers, identified by the review search strategy, for relevancy. Two review authors independently assessed the full text of all potentially relevant trials for eligibility, completed the data extraction and assessed the studies for risk of bias using The Cochrane Collaboration's 'Risk of bias' tool. We requested missing data from one author but the data were no longer available. The outcomes are reported narratively: we performed no meta-analyses because of the heterogeneity of the available data.
We identified three new studies in this update of the review. In total seven studies were eligible for inclusion, three were ongoing RCTs and four were completed studies. The four completed studies were included in the original review and the three ongoing studies were included in this update. We did not identify any RCTs that compared TXA with EACA.Of the four completed studies, one cross-over TXA study (eight participants) was excluded from the outcome analysis because it had very flawed study methodology. Data from the other three studies were all at unclear risk of bias due to lack of reporting of study methodology.Three studies (two TXA (12 to 56 participants), one EACA (18 participants) reported in four articles (published 1983 to 1995) were included in the narrative review. All three studies compared the drug with placebo. All three studies included adults with acute leukaemia receiving chemotherapy. One study (12 participants) only included participants with acute promyelocytic leukaemia. None of the studies included children. One of the three studies reported funding sources and this study was funded by a charity.We are uncertain whether antifibrinolytics reduce the risk of bleeding (three studies; 86 participants; very low-quality evidence). Only one study reported the number of bleeding events per participant and there was no difference in the number of bleeding events seen during induction or consolidation chemotherapy between TXA and placebo (induction; 38 participants; mean difference (MD) 1.70 bleeding events, 95% confidence interval (CI) -0.37 to 3.77: consolidation; 18 participants; MD -1.50 bleeding events, 95% CI -3.25 to 0.25; very low-quality evidence). The two other studies suggested bleeding was reduced in the antifibrinolytic study arm, but this was statistically significant in only one of these two studies.Two studies reported thromboembolism and no events occurred (68 participants, very low-quality evidence).All three studies reported a reduction in platelet transfusion usage (three studies, 86 participants; very low-quality evidence), but this was reported in different ways and no meta-analysis could be performed. No trials reported the number of platelet transfusions per participant. Only one study reported the number of platelet components per participant and there was a reduction in the number of platelet components per participant during consolidation chemotherapy but not during induction chemotherapy (consolidation; 18 participants; MD -5.60 platelet units, 95% CI -9.02 to -2.18: induction; 38 participants, MD -1.00 platelet units, 95% CI -9.11 to 7.11; very low-quality evidence).Only one study reported adverse events of TXA as an outcome measure and none occurred. One study stated side effects of EACA were minimal but no further information was provided (two studies, 74 participants, very low-quality evidence).None of the studies reported on the following pre-specified outcomes: overall mortality, adverse events of transfusion, disseminated intravascular coagulation (DIC) or quality of life (QoL).
AUTHORS' CONCLUSIONS: Our results indicate that the evidence available for the use of antifibrinolytics in haematology patients is very limited. The trials were too small to assess whether or not antifibrinolytics decrease bleeding. No trials reported the number of platelet transfusions per participant. The trials were too small to assess whether or not antifibrinolytics increased the risk of thromboembolic events or other adverse events. There are three ongoing RCTs (1276 participants) due to be completed in 2017 and 2020.
血液系统疾病患者由于血小板减少(血小板计数降低),经常面临严重出血或危及生命的出血风险。尽管一旦血小板计数低于某个阈值,通常会使用预防性血小板输注来预防出血,但血小板输注并非没有风险,不良事件可能会危及生命。预防性血小板输注的一种可能辅助手段是使用抗纤维蛋白溶解剂,特别是赖氨酸类似物氨甲环酸(TXA)和ε-氨基己酸(EACA)。这是对2013年首次发表的Cochrane系统评价的更新。
确定抗纤维蛋白溶解剂(赖氨酸类似物)在预防血液系统疾病患者出血方面的疗效和安全性。
我们在Cochrane对照试验中心注册库(Cochrane图书馆2016年第3期)、MEDLINE(1946年起)、Embase(1974年起)、CINAHL(1937年起)、输血证据图书馆(1950年起)以及截至2016年3月7日的正在进行的试验数据库中检索随机对照试验(RCT)。
我们纳入了涉及血液系统疾病患者的RCT,这些患者通常需要预防性血小板输注来预防出血。我们仅纳入了涉及使用赖氨酸类似物TXA和EACA的试验。
两位综述作者独立筛选所有通过综述检索策略识别出的电子文献引用和论文摘要,以确定其相关性。两位综述作者独立评估所有潜在相关试验的全文是否符合纳入标准,并完成数据提取,使用Cochrane协作网的“偏倚风险”工具评估研究的偏倚风险。我们向一位作者索要缺失数据,但数据已无法获取。结果采用叙述性报告:由于现有数据的异质性,我们未进行荟萃分析。
在本次综述更新中,我们识别出三项新研究。总共有七项研究符合纳入标准,三项是正在进行的RCT,四项是已完成的研究。四项已完成的研究包含在原始综述中,三项正在进行的研究包含在本次更新中。我们未识别出任何比较TXA和EACA的RCT。在四项已完成的研究中,一项交叉设计的TXA研究(8名参与者)由于研究方法存在严重缺陷,被排除在结果分析之外。由于缺乏对研究方法的报告,其他三项研究的数据偏倚风险均不明确。三项研究(两项TXA研究(12至56名参与者),一项EACA研究(18名参与者),发表于四篇文章(发表于1983年至1995年))被纳入叙述性综述。所有三项研究均将药物与安慰剂进行比较。所有三项研究均纳入了接受化疗的成年急性白血病患者。一项研究(12名参与者)仅纳入了急性早幼粒细胞白血病患者。所有研究均未纳入儿童。三项研究中有一项报告了资金来源,该研究由一家慈善机构资助。我们不确定抗纤维蛋白溶解剂是否能降低出血风险(三项研究;86名参与者;极低质量证据)。只有一项研究报告了每位参与者的出血事件数量,在诱导化疗或巩固化疗期间,TXA组和安慰剂组的出血事件数量没有差异(诱导化疗;38名参与者;平均差(MD)1.70次出血事件,95%置信区间(CI)-0.37至3.77;巩固化疗;18名参与者;MD -1.50次出血事件,95%CI -3.25至0.25;极低质量证据)。另外两项研究表明抗纤维蛋白溶解剂治疗组的出血有所减少,但在这两项研究中只有一项具有统计学意义。两项研究报告了血栓栓塞事件,未发生此类事件(68名参与者,极低质量证据)。所有三项研究均报告血小板输注用量减少(三项研究,86名参与者;极低质量证据),但报告方式不同,无法进行荟萃分析。没有试验报告每位参与者的血小板输注次数。只有一项研究报告了每位参与者的血小板成分数量,在巩固化疗期间每位参与者的血小板成分数量减少,但在诱导化疗期间未减少(巩固化疗;18名参与者;MD -5.60个血小板单位,95%CI -9.02至-2.18;诱导化疗;38名参与者,MD -1.00个血小板单位,95%CI -9.11至7.1:极低质量证据)。只有一项研究将TXA的不良事件作为结局指标进行报告,未发生不良事件。一项研究称EACA的副作用极小,但未提供进一步信息(两项研究,74名参与者,极低质量证据)。没有研究报告以下预先设定的结局:总死亡率、输血不良事件、弥散性血管内凝血(DIC)或生活质量(QoL)。
我们的结果表明,血液学患者使用抗纤维蛋白溶解剂的现有证据非常有限。试验规模太小,无法评估抗纤维蛋白溶解剂是否能减少出血。没有试验报告每位参与者的血小板输注次数。试验规模太小,无法评估抗纤维蛋白溶解剂是否会增加血栓栓塞事件或其他不良事件的风险。有三项正在进行的RCT(1276名参与者)将于2017年和2020年完成。
