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[动脉和静脉性脑缺血的治疗。专家建议:重症监护病房中的卒中管理]

[Treatment of arterial and venous brain ischemia. Experts' recommendations: stroke management in the intensive care unit].

作者信息

Calvet D, Bracard S, Mas J-L

机构信息

Service de neurologie et unité neurovasculaire, INSERM UMR 894, université Paris Descartes, centre hospitalier Sainte-Anne, 1 rue Cabanis, Paris cedex 14, France.

出版信息

Rev Neurol (Paris). 2012 Jun;168(6-7):512-21. doi: 10.1016/j.neurol.2012.01.587. Epub 2012 May 28.

Abstract

With thrombolysis, intravenous alteplase (0.9 mg/kg body weight, maximum 90 mg), with 10% of the dose given as a bolus followed by a 60-minute infusion, is recommended within 4.5 hours of onset of ischemic stroke. When indicated, intravenous thrombolysis must be initiated as soon as possible. It is possible to use intravenous alteplase in patients with seizures at stroke onset, if the neurological deficit is related to acute cerebral ischemia. Intravenous alteplase can be discussed for use on a case-by-case basis, according to risk of bleeding, in selected patients under 18 years and over 80 years of age, although for the current European recommendations this would be an off-label use. In hospitals with a stroke unit, intravenous thrombolysis is prescribed by a neurologist (current French labelling) or a physician having the French certification for neurovascular diseases (outside the current French labelling). The patient must be monitored in the stroke unit or in case of multiple organ failure in an intensive and critical care unit. In hospitals without a stroke unit, thrombolysis must be decided by the neurologist from the corresponding stroke unit via telemedicine. It is recommended to perform brain imaging 24 hours after thromboysis. Intra-arterial thrombolysis can be contemplated on a case-by-case basis after multidisciplinary discussion within a 6-hour time window for patients with acute middle cerebral artery or carotid occlusions, and within a larger time window for patients with basilar artery occlusion, because of their very poor spontaneous prognosis. Mechanical thrombectomy can also be contemplated in the same situations. With antiplatelet agents, it is recommended that patients receive aspirin (160 mg-325 mg) within 48 hours of ischemic stroke onset. When thrombolysis is performed or contemplated, it is recommended to delay the initiation of aspirin or other antithrombotic drugs for 24 hours. The use of antiplatelet agents that inhibit the glycoprotein IIb/IIIa receptor is not recommended. Urgent anticoagulation using heparin, low-molecular-weight heparins or danaparoid with the goal to treat ischemic stroke patients is not recommended. Secondary prevention by anticoagulation can be used, immediately or within the first days, after minor ischemic stroke or TIA in patients with a high risk for cardioembolism, if uncontrolled hypertension is absent. In patients with large infarcts and a high risk for cardioembolism, the timing for initiating anticoagulation must be decided on a case-by-case basis. In patients with anticoagulation who had an ischemic stroke, the decision to temporarily stop or maintain anticoagulation must be made on a case-by-case basis, depending on thromboembolic risk, level of anticoagulation at stroke onset and estimated risk of hemorrhagic transformation. It is not recommended to use neuroprotective agents in ischemic stroke patients. Patients with cerebral venous thrombosis must be treated with therapeutic doses of heparin, even in case of concomitant intracranial hemorrhage related to cerebral venous thrombosis. If the patient's status worsens despite adequate anticoagulation, thrombolysis may be used in selected cases. The optimal administration route (local or intravenous), thrombolytic agent (urokinase or alteplase) and dose are unknown. There is currently no recommendation with regard to local thrombolytic therapy in patients with dural sinus thrombosis. Urgent blood transfusions are recommended to reduce hemoglobin S to <30% in patients with sickle cell disease and acute ischemic stroke.

摘要

对于缺血性卒中发作4.5小时内的患者,推荐进行溶栓治疗,静脉注射阿替普酶(0.9mg/kg体重,最大剂量90mg),其中10%的剂量作为静脉推注,随后进行60分钟的输注。如有指征,必须尽快开始静脉溶栓治疗。如果神经功能缺损与急性脑缺血相关,卒中发作时伴有癫痫发作的患者也可使用静脉注射阿替普酶。对于18岁以下和80岁以上的特定患者,可根据出血风险逐案讨论是否使用静脉注射阿替普酶,不过按照目前欧洲的建议,这属于超适应证用药。在设有卒中单元的医院,由神经科医生(根据当前法国标签)或具有法国神经血管疾病认证的医生(超出当前法国标签范围)开具静脉溶栓治疗的处方。患者必须在卒中单元或在重症监护病房出现多器官功能衰竭时接受监测。在没有卒中单元的医院,必须由相应卒中单元的神经科医生通过远程医疗来决定是否进行溶栓治疗。建议在溶栓治疗24小时后进行脑部成像检查。对于急性大脑中动脉或颈动脉闭塞的患者,可在6小时时间窗内进行多学科讨论后逐案考虑动脉内溶栓治疗;对于基底动脉闭塞的患者,由于其自然预后非常差,可在更大的时间窗内进行动脉内溶栓治疗。在相同情况下也可考虑机械取栓治疗。对于抗血小板药物,建议患者在缺血性卒中发作48小时内服用阿司匹林(160mg - 325mg)。当进行或考虑进行溶栓治疗时,建议将阿司匹林或其他抗血栓药物的起始时间推迟24小时。不建议使用抑制糖蛋白IIb/IIIa受体的抗血小板药物。不建议使用肝素、低分子肝素或达那肝素进行紧急抗凝治疗以治疗缺血性卒中患者。对于有心脏栓塞高风险的患者,如果没有未控制的高血压,在轻度缺血性卒中或短暂性脑缺血发作后,可立即或在最初几天内使用抗凝进行二级预防。对于大面积梗死且有心脏栓塞高风险的患者,开始抗凝治疗的时机必须逐案决定。对于正在接受抗凝治疗且发生缺血性卒中的患者,必须根据血栓栓塞风险、卒中发作时的抗凝水平以及出血转化的估计风险逐案决定是暂时停用还是维持抗凝治疗。不建议在缺血性卒中患者中使用神经保护剂。患有脑静脉血栓形成的患者必须接受治疗剂量的肝素治疗,即使伴有与脑静脉血栓形成相关的颅内出血。如果尽管进行了充分的抗凝治疗患者病情仍恶化,在某些选定的病例中可使用溶栓治疗。最佳给药途径(局部或静脉)、溶栓剂(尿激酶或阿替普酶)和剂量尚不清楚。目前对于硬脑膜窦血栓形成患者的局部溶栓治疗尚无推荐。对于镰状细胞病和急性缺血性卒中患者,建议紧急输血以将血红蛋白S降至<30%。

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