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颅内出血情况下华法林的快速逆转:血浆、重组活化因子 VII 和凝血酶原复合物浓缩物的比较。

Rapid Warfarin reversal in the setting of intracranial hemorrhage: a comparison of plasma, recombinant activated factor VII, and prothrombin complex concentrate.

机构信息

Department of Pharmacy, Kaiser Permanente Medical Center, San Francisco, California, USA.

Department of Neurosurgery/Neuroscience, Kaiser Permanente Medical Center, Redwood City, California, USA.

出版信息

World Neurosurg. 2014 Jan;81(1):110-5. doi: 10.1016/j.wneu.2012.12.002. Epub 2012 Dec 5.

Abstract

OBJECTIVE

To compare the safety and effectiveness of three methods of reversing coagulopathic effects of warfarin in patients with potentially life-threatening intracranial hemorrhage.

METHODS

A retrospective electronic medical record review of 63 patients with warfarin-related intracranial hemorrhage between 2007 and 2010 in an integrated health care delivery system was conducted. The three methods of rapid warfarin reversal were fresh-frozen plasma (FFP), activated factor VII (FVIIa; NovoSevenRT [Novo Nordisk, Bagsværd, Denmark]), and prothrombin complex concentrate (PCC; BebulinVH [Baxter, Westlake Village, California, USA], ProfilnineSD [Grifols, North Carolina, USA]), each used adjunctively with vitamin K (Vit K, phytonadione). We determined times from reversal agent order to laboratory evidence of warfarin reversal (international normalized ratio [INR]) in the first 48 hours and compared INR rebound rates and complications in the first 48 hours.

RESULTS

Reversal with FFP took more than twice as long compared with FVIIa or PCC. To reach an INR of 1.3, mean (±SD) reversal times were 1933 ± 905 minutes for FFP, 784 ± 926 minutes for FVIIa, and 980 ± 1021 minutes for PCC (P < 0.001; P < 0.01 between FFP and FVIIa, P < 0.05 between FFP and PCC). INR rebound occurred in 0 of 31 patients for FFP, 4 of 8 for FVIIa, and 0 of 7 for PCC (P = 0.001). Complications were uncommon. FVIIa was 15 and 3.5 times as expensive as FFP and PCC, respectively.

CONCLUSION

As an adjunct to Vit K for rapid warfarin reversal, FVIIa and PCC appear more effective than FFP. Either FVIIa or PCC are reasonable options for reversal, but FVIIa is considerably more expensive and may have greater risk of INR rebound.

摘要

目的

比较三种逆转华法林致危及生命颅内出血患者凝血异常效果的安全性和有效性。

方法

对 2007 年至 2010 年在综合医疗服务系统中发生华法林相关性颅内出血的 63 例患者进行了回顾性电子病历研究。三种快速逆转华法林的方法为新鲜冷冻血浆(FFP)、活化因子 VII(FVIIa;NovoSevenRT[Novo Nordisk, Bagsværd,丹麦])和凝血酶原复合物浓缩物(PCC;BebulinVH[Baxter,加利福尼亚州西湖村]、ProfilnineSD[Grifols,北卡罗来纳州]),每种方法均联合应用维生素 K(Vit K,叶绿醌)。我们确定了从逆转剂下订单到前 48 小时实验室检测到华法林逆转(国际标准化比值[INR])的时间,并比较了前 48 小时内 INR 反弹率和并发症。

结果

与 FVIIa 或 PCC 相比,FFP 逆转时间超过两倍。要达到 INR 为 1.3,FFP 的平均(±SD)逆转时间为 1933 ± 905 分钟,FVIIa 为 784 ± 926 分钟,PCC 为 980 ± 1021 分钟(P < 0.001;FFP 与 FVIIa 之间 P < 0.01,FFP 与 PCC 之间 P < 0.05)。FFP 组 31 例患者中无 INR 反弹,FVIIa 组 8 例中有 4 例,PCC 组 7 例中有 0 例(P = 0.001)。并发症并不常见。FVIIa 分别比 FFP 和 PCC 贵 15 倍和 3.5 倍。

结论

作为 Vit K 辅助快速逆转华法林的手段,FVIIa 和 PCC 似乎比 FFP 更有效。FVIIa 或 PCC 都是逆转的合理选择,但 FVIIa 价格昂贵得多,且 INR 反弹的风险可能更大。

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