Brenner Amy, Afolabi Adefemi, Ahmad Syed Masroor, Arribas Monica, Chaudhri Rizwana, Coats Timothy, Cuzick Jack, Gilmore Ian, Hawkey Christopher, Jairath Vipul, Javaid Kiran, Kayani Aasia, Mutti Muttiullah, Nadeem Muhammad Arif, Shakur-Still Haleema, Stanworth Simon, Veitch Andrew, Roberts Ian
Clinical Trials Unit, Department of Population Health, London School of Hygiene and Tropical Medicine, Keppel Street, London, WC1E 7HT, UK.
Department of Surgery, College of Medicine, University of Ibadan, University College Hospital, Queen Elizabeth Road, Ibadan, 200001, Nigeria.
Trials. 2019 Jul 30;20(1):467. doi: 10.1186/s13063-019-3561-7.
Acute gastrointestinal (GI) bleeding is an important cause of mortality worldwide. Bleeding can occur from the upper or lower GI tract, with upper GI bleeding accounting for most cases. The main causes include peptic ulcer/erosive mucosal disease, oesophageal varices and malignancy. The case fatality rate is around 10% for upper GI bleeding and 3% for lower GI bleeding. Rebleeding affects 5-40% of patients and is associated with a four-fold increased risk of death. Tranexamic acid (TXA) decreases bleeding and the need for blood transfusion in surgery and reduces death due to bleeding in patients with trauma and postpartum haemorrhage. It reduces bleeding by inhibiting the breakdown of fibrin clots by plasmin. Due to the methodological weaknesses and small size of the existing trials, the effectiveness and safety of TXA in GI bleeding is uncertain. The Haemorrhage ALleviation with Tranexamic acid - Intestinal system (HALT-IT) trial aims to provide reliable evidence about the effects of TXA in acute upper and lower GI bleeding.
The HALT-IT trial is an international, randomised, double-blind, placebo-controlled trial of tranexamic acid in 12,000 adults (increased from 8000) with acute upper or lower GI bleeding. Eligible patients are randomly allocated to receive TXA (1-g loading dose followed by 3-g maintenance dose over 24 h) or matching placebo. The main analysis will compare those randomised to TXA with those randomised to placebo on an intention-to-treat basis, presenting the results as effect estimates (relative risks) and confidence intervals. The primary outcome is death due to bleeding within 5 days of randomisation and secondary outcomes are: rebleeding; all-cause and cause-specific mortality; thromboembolic events; complications; endoscopic, radiological and surgical interventions; blood transfusion requirements; disability (defined by a measure of patient's self-care capacity); and number of days spent in intensive care or high-dependency units. Subgroup analyses for the primary outcome will consider time to treatment, location of bleeding, cause of bleed and clinical Rockall score.
We present the statistical analysis of the HALT-IT trial. This plan was published before the treatment allocation was unblinded.
Current Controlled Trials, ID: ISRCTN11225767. Registered on 3 July 2012; Clinicaltrials.gov, ID: NCT01658124. Registered on 26 July 2012.
急性胃肠道(GI)出血是全球范围内一个重要的死亡原因。出血可发生在上消化道或下消化道,其中上消化道出血占大多数病例。主要病因包括消化性溃疡/糜烂性黏膜病、食管静脉曲张和恶性肿瘤。上消化道出血的病死率约为10%,下消化道出血为3%。再出血影响5% - 40%的患者,且死亡风险增加四倍。氨甲环酸(TXA)可减少手术中的出血及输血需求,并降低创伤和产后出血患者因出血导致的死亡。它通过抑制纤溶酶对纤维蛋白凝块的分解来减少出血。由于现有试验存在方法学缺陷且规模较小,TXA在胃肠道出血中的有效性和安全性尚不确定。氨甲环酸减轻肠道系统出血(HALT - IT)试验旨在提供关于TXA在急性上消化道和下消化道出血中作用的可靠证据。
HALT - IT试验是一项国际、随机、双盲、安慰剂对照试验,纳入12000名(从8000名增加)患有急性上消化道或下消化道出血的成年人,对其使用氨甲环酸。符合条件的患者被随机分配接受TXA(1克负荷剂量,随后在24小时内给予3克维持剂量)或匹配的安慰剂。主要分析将在意向性治疗基础上比较随机接受TXA与随机接受安慰剂的患者,结果以效应估计值(相对风险)和置信区间呈现。主要结局是随机分组后5天内因出血导致的死亡,次要结局包括:再出血;全因死亡率和特定病因死亡率;血栓栓塞事件;并发症;内镜、放射学和外科干预;输血需求;残疾(通过患者自我护理能力的测量来定义);以及在重症监护或高依赖病房的住院天数。主要结局的亚组分析将考虑治疗时间、出血部位、出血原因和临床Rockall评分。
我们展示了HALT - IT试验的统计分析。该方案在治疗分配未揭盲前已发表。
当前受控试验,编号:ISRCTN11225767。于2012年7月3日注册;Clinicaltrials.gov,编号:NCT01658124。于2012年7月26日注册。
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