Raskob Gary E, van Es Nick, Segers Annelise, Angchaisuksiri Pantep, Oh Doyeun, Boda Zoltan, Lyons Roger M, Meijer Karina, Gudz Ivan, Weitz Jeffrey I, Zhang George, Lanz Hans, Mercuri Michele F, Büller Harry R
College of Public Health, University of Oklahoma Health Sciences Center, Oklahoma City, OK, USA.
Department of Vascular Medicine, Academic Medical Center, Amsterdam, Netherlands.
Lancet Haematol. 2016 Aug;3(8):e379-87. doi: 10.1016/S2352-3026(16)30057-6. Epub 2016 Jul 1.
Venous thromboembolism occurs commonly in patients with cancer. Direct oral anticoagulants are non-inferior to conventional anticoagulants for the treatment of venous thromboembolism. We hypothesised that edoxaban, a direct oral inhibitor of activated clotting factor Xa, might be more suitable than conventional anticoagulants in the management of cancer-associated venous thromboembolism. The aim of this study was to assess the efficacy and safety of edoxaban compared with warfarin in a subgroup of patients with cancer enrolled in the Hokusai-VTE trial.
We did a prespecified subgroup analysis in August, 2013, and a post-hoc analysis of non-inferiority and safety in March, 2016, of the patients with cancer enrolled in the randomised, double-blind, double-dummy, multicentre, Hokusai-VTE trial done between Jan 28, 2010, and Oct 31, 2012. In this study, patients aged at least 18 years with acute symptomatic deep-vein thrombosis or acute symptomatic pulmonary embolism (with or without deep-vein thrombosis) were assigned to receive edoxaban 60 mg once per day (or 30 mg once per day for patients with a creatinine clearance of 30-50 mL/min, bodyweight <60 kg, or who were receiving concomitant treatment with the P-glycoprotein inhibitors quinidine or verapamil) or warfarin (dose adjusted to maintain the international normalised ratio between 2·0 and 3·0) or placebos for either group for at least 3 months up to 12 months. All patients received initial therapy with open-label enoxaparin or unfractionated heparin for at least 5 days. Edoxoban (or placebo) was started after discontinuation of initial heparin; warfarin (or placebo) started concurrently with the study regimen of heparin. In our analysis we examined data for a subgroup of these patients who had a history of cancer or who had been categorised as having active cancer by the study physician at the time of enrolment. Additionally, all patients with a history of cancer were reviewed post hoc and categorised according to the presence or absence of active cancer. The primary efficacy outcome was the proportion of these patients with symptomatic recurrent venous thromboembolism during the 12-month study period, analysed in the modified intention-to-treat population, with an upper limit of the CI for the hazard ratio (HR) of 1·5. The principal safety outcome was the proportion of patients who had clinically relevant bleeding in the population of patients who received at least one dose of the study drug. This study is registered with ClinicalTrials.gov, number NCT00986154.
Of 771 patients with cancer enrolled in the trial, 378 were assigned to edoxaban and 393 to warfarin. Recurrent venous thromboembolism occurred in 14 (4%) of 378 patients given edoxaban and in 28 (7%) of 393 patients given warfarin (hazard ratio [HR] 0·53, 95% CI 0·28-1·00; p=0·0007). The upper limit of this 95% CI did not exceed the non-inferiority margin of 1·5 that was prespecified for the trial. Clinically relevant bleeding (major or non-major) occurred in 47 (12%) of 378 patients who received edoxaban and in 74 (19%) of 393 patients who received warfarin; HR for clinically relevant bleeding 0·64, 95% CI 0·45-0·92; p=0·017. Major bleeding occurred in ten (3%) of 378 patients with a history of cancer who received edoxaban and in 13 (3%) of 393 who received warfarin (HR 0·80, 95% CI 0·35-1·83).
Edoxaban might be as effective as warfarin for the treatment of patients with cancer with venous thromboembolism, and with less clinically relevant bleeding. Additional clinical trials of edoxaban versus low-molecular-weight heparin for the treatment of venous thromboembolism in patients with cancer are warranted.
Daiichi Sankyo.
静脉血栓栓塞在癌症患者中很常见。直接口服抗凝剂在治疗静脉血栓栓塞方面不劣于传统抗凝剂。我们推测,阿哌沙班(一种活化凝血因子Xa的直接口服抑制剂)在管理癌症相关静脉血栓栓塞方面可能比传统抗凝剂更合适。本研究的目的是在参加“北陆-VTE”试验的癌症患者亚组中评估阿哌沙班与华法林相比的疗效和安全性。
我们于2013年8月进行了一项预先设定的亚组分析,并于2016年3月对2010年1月28日至2012年10月31日进行的随机、双盲、双模拟、多中心“北陆-VTE”试验中入组的癌症患者进行了非劣效性和安全性的事后分析。在本研究中,年龄至少18岁的急性症状性深静脉血栓形成或急性症状性肺栓塞(伴或不伴深静脉血栓形成)患者被分配接受阿哌沙班60mg每日一次(肌酐清除率为30-50mL/min、体重<60kg或正在接受P-糖蛋白抑制剂奎尼丁或维拉帕米联合治疗的患者为30mg每日一次)或华法林(调整剂量以维持国际标准化比值在2.0至3.0之间)或两组的安慰剂,持续至少3个月至12个月。所有患者均接受至少5天的开放标签依诺肝素或普通肝素初始治疗。在停用初始肝素后开始使用阿哌沙班(或安慰剂);华法林(或安慰剂)与肝素的研究方案同时开始。在我们的分析中,我们检查了这些患者亚组的数据,这些患者有癌症病史或在入组时被研究医生归类为患有活动性癌症。此外,对所有有癌症病史的患者进行事后审查,并根据是否存在活动性癌症进行分类。主要疗效结局是在12个月研究期间这些有症状复发性静脉血栓栓塞患者的比例,在改良意向性治疗人群中进行分析,风险比(HR)的CI上限为1.5。主要安全结局是在接受至少一剂研究药物的患者人群中发生临床相关出血的患者比例。本研究已在ClinicalTrials.gov注册,编号为NCT00986154。
在试验入组的771例癌症患者中,378例被分配接受阿哌沙班,393例被分配接受华法林。接受阿哌沙班治疗的378例患者中有14例(4%)发生复发性静脉血栓栓塞,接受华法林治疗的393例患者中有28例(7%)发生复发性静脉血栓栓塞(风险比[HR]0.53,95%CI0.28-1.00;p=0.0007)。该95%CI的上限未超过试验预先设定的非劣效性界值1.5。接受阿哌沙班治疗的378例患者中有47例(12%)发生临床相关出血(大出血或非大出血),接受华法林治疗的393例患者中有74例(19%)发生临床相关出血;临床相关出血的HR为0.64,95%CI为0.45-0.92;p=0.017。有癌症病史的378例接受阿哌沙班治疗的患者中有10例(3%)发生大出血,393例接受华法林治疗的患者中有13例(3%)发生大出血(HR0.80,95%CI0.35-1.83)。
阿哌沙班在治疗患有静脉血栓栓塞的癌症患者方面可能与华法林一样有效,且临床相关出血较少。有必要进行阿哌沙班与低分子肝素治疗癌症患者静脉血栓栓塞的额外临床试验。
第一三共株式会社。
