Surgical Unit, Khon Kaen hospital, Khon Kaen, Thailand.
BMC Emerg Med. 2013 Nov 22;13:20. doi: 10.1186/1471-227X-13-20.
Traumatic brain injury (TBI) is commonly accompanied by intracranial bleeding which can worsen after hospital admission. Tranexamic acid (TXA) has been shown to reduce bleeding in elective surgery and there is evidence that short courses of TXA can reduce rebleeding in spontaneous intracranial haemorrhage. We aimed to determine the effectiveness and safety of TXA in preventing progressive intracranial haemorrhage in TBI.
This is a double blinded, placebo controlled randomized trial. We enrolled 238 patients older than 16 years with moderate to severe TBI (post-resuscitation Glasgow Coma Scale (GCS) 4 to 12) who had a computerized tomography (CT) brain scan within eight hours of injury and in whom there was no immediate indication for surgery. We excluded patients if they had a coagulopathy or a serum creatinine over than 2.0 milligrams%. The treatment was a single dose of 2 grams of TXA in addition to other standard treatments. The primary outcome was progressive intracranial haemorrhage (PIH) which was defined as an intracranial haemorrhage seen on the second CT scan that was not seen on the first CT scan, or an intracranial haemorrhage seen on the first scan that had expanded by 25% or more on any dimension (height, length, or width) on the second scan.
Progressive intracranial haemorrhage was present in 21 (18%) of 120 patients allocated to TXA and in 32 (27%) of 118 patients allocated to placebo. The difference was not statistically significant [RR = 0.65 (95% CI 0.40 to 1.05)]. There were no significant difference in the risk of death from all causes in patients allocated to TXA compared with placebo [RR = 0.69 (95% CI 0.35 to 1.39)] and the risk of unfavourable outcome on the Glasgow Outcome Scale [RR = 0.76 (95% CI 0.46 to 1.27)]. There was no evidence of increased risk of thromboembolic events in those patients allocated to TXA.
TXA may reduce PIH in patients with TBI; however, the difference was not statistically significant in this trial. Large clinical trials are needed to confirm and to assess the effect of TXA on death or disability after TBI.
创伤性脑损伤(TBI)通常伴有颅内出血,这种出血在入院后可能会恶化。氨甲环酸(TXA)已被证明可减少择期手术中的出血,并有证据表明短疗程 TXA 可减少自发性颅内出血的再出血。我们旨在确定 TXA 在预防 TBI 进行性颅内出血中的有效性和安全性。
这是一项双盲、安慰剂对照的随机试验。我们招募了 238 名年龄在 16 岁以上、格拉斯哥昏迷量表(GCS)评分 4 至 12 分的中度至重度 TBI 患者,这些患者在受伤后 8 小时内进行了计算机断层扫描(CT)脑部扫描,并且没有立即进行手术的指征。如果患者有凝血障碍或血清肌酐超过 2.0 毫克/分升,则将其排除在外。治疗是在其他标准治疗的基础上,单次给予 2 克 TXA。主要结局是进行性颅内出血(PIH),定义为第二次 CT 扫描中可见的颅内出血,而第一次 CT 扫描中未见,或第一次扫描中可见的颅内出血,第二次扫描中在任何维度(高度、长度或宽度)上扩大了 25%或更多。
在接受 TXA 治疗的 120 名患者中有 21 名(18%)和接受安慰剂治疗的 118 名患者中有 32 名(27%)出现进行性颅内出血。差异无统计学意义[RR=0.65(95%CI 0.40 至 1.05)]。与安慰剂相比,接受 TXA 治疗的患者因任何原因死亡的风险无显著差异[RR=0.69(95%CI 0.35 至 1.39)],格拉斯哥结局量表的不良结局风险也无显著差异[RR=0.76(95%CI 0.46 至 1.27)]。没有证据表明接受 TXA 治疗的患者血栓栓塞事件的风险增加。
TXA 可能减少 TBI 患者的 PIH;然而,本试验中差异无统计学意义。需要进行大型临床试验来证实和评估 TXA 对 TBI 后死亡或残疾的影响。
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