阿昔单抗(ReoPro)在颅内动脉瘤管道分流治疗中急性术中血栓栓塞并发症的剂量策略。

Q1 Medicine Interventional Neurology Pub Date : 2018-04-01 Epub Date: 2018-02-27 DOI:10.1159/000486458
Li-Mei Lin, Bowen Jiang, Jessica K Campos, Narlin B Beaty, Matthew T Bender, Rafael J Tamargo, Judy Huang, Geoffrey P Colby, Alexander L Coon
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引用次数: 9

摘要

背景:管道栓塞装置(PED)分流是一种有效的神经血管内方法,越来越多地被接受用于治疗脑动脉瘤。急性原位血栓形成是PED手术的已知并发症。关于使用阿昔单抗(ReoPro)治疗PED患者急性血栓形成的分流文献经验有限。方法:回顾性收集在PED分流治疗颅内动脉瘤过程中接受动脉内(IA) ReoPro伴或不伴静脉(IV)输注的患者资料。结果:共有30例患者,平均年龄为56.7岁(范围36-84),平均动脉瘤大小为8.6 mm(范围2-25),在PED治疗过程中发现术中血栓栓塞并发症。所有病例均给予IA ReoPro,其中20例接受5mg剂量的增量,10例接受0.125 mg/kg的IA剂量(心脏剂量的一半)。100%的病例实现了完全或部分再通。22例残余血栓患者术后静脉滴注ReoPro, 0.125 μg/kg/min,持续12 h。术后,18例患者从氯吡格雷(Plavix)过渡到普拉格雷(effent)。大多数病例(23/30;77%)出院回家。术中颅内出血2例(7%),影像学梗死4例(13%),初次出院时总死亡率为0%。临床随访28/30例。平均随访时间为11.7个月,其中23/28(82%)的患者改良Rankin量表评分为0分。结论:对于PED治疗过程中的急性术中血栓栓塞并发症,IA ReoPro给药是一种有效且安全的抢救策略。使用5mg增量或0.125 mg/kg IA(心脏剂量的一半)的给药策略可以提供高的再通率,低的出血性并发症和长期发病率。
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Abciximab (ReoPro) Dosing Strategy for the Management of Acute Intraprocedural Thromboembolic Complications during Pipeline Flow Diversion Treatment of Intracranial Aneurysms.

Background: Flow diversion with the Pipeline embolization device (PED) is an effective neuro-endovascular method and increasingly accepted for the treatment of cerebral aneurysms. Acute in situ thrombosis is a known complication of PED procedures. There is limited experience in the flow diversion literature on the use of abciximab (ReoPro) for the management of acute thrombus formation in PED cases.

Methods: Data were collected retrospectively on patients who received intra-arterial (IA) ReoPro with or without subsequent intravenous (IV) infusion during PED flow diversion treatment of intracranial aneurysms.

Results: A total of 30 cases in patients with a mean age of 56.7 years (range 36-84) and a mean aneurysm size of 8.6 mm (range 2-25) were identified to have intraprocedural thromboembolic complications during PED treatment. IA ReoPro was administered in all cases, with 20 cases receiving increments of 5-mg boluses and 10 cases receiving a 0.125 mg/kg IA bolus (half cardiac dosing). Complete or partial recanalization was achieved in 100% of the cases. IV ReoPro infusion at 0.125 μg/kg/min for 12 h was administered postprocedurally in 22 cases with a residual thrombus. Postprocedurally, 18 patients were transitioned from clopidogrel (Plavix) to prasugrel (Effient). The majority of the cases (23/30; 77%) were discharged home. Periprocedural intracranial hemorrhage was noted in 2 cases (7%) and radiographic infarct was noted in 4 cases (13%), with an overall mortality of 0% at the time of initial discharge. Clinical follow-up was available for 28/30 patients. The average duration of follow-up was 11.7 months, at which time 23/28 (82%) of the patients had a modified Rankin Scale score of 0.

Conclusions: IA ReoPro administration is an effective and safe rescue strategy for the management of acute intraprocedural thromboembolic complications during PED treatment. Using a dosing strategy of either 5-mg increments or a 0.125 mg/kg IA bolus (half cardiac dosing) can provide high rates of recanalization with low rates of hemorrhagic complications and long-term morbidity.

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Interventional Neurology
Interventional Neurology CLINICAL NEUROLOGY-
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