Kramer Andreas H, Le Roux Peter
Department of Critical Care Medicine & Clinical Neurosciences, University of Calgary, Ground Floor, McCaig Tower, 3134 Hospital Dr NW, Calgary, AB, T2N 2T9, Canada.
Curr Treat Options Neurol. 2012 Apr;14(2):150-163. doi: 10.1007/s11940-012-0167-8. Epub 2012 Feb 8.
Anemia develops in about 50% of patients hospitalized with traumatic brain injury (TBI) and is recognized as a cause of secondary brain injury. This review examines the effects of anemia and transfusion on TBI patients through a literature search to identify original research on anemia and transfusion in TBI, the effects of transfusion on brain physiology, and the role of erythropoietin or hemoglobin-based blood substitutes (HBBSs). However, the amount of high-quality, prospective data available to help make decisions about when TBI patients should be transfused is very small. Randomized transfusion trials have involved far too few TBI patients to reach definitive conclusions. Thus, it is hardly surprising that there is widespread practice variation. In our opinion, a hemoglobin transfusion threshold of 7 g/dL cannot yet be considered safe for TBI patients admitted to hospital, and in particular to the ICU, as it is for other critically ill patients. Red blood cell transfusions often have immediate, seemingly beneficial effects on cerebral physiology, but the magnitude of this effect may depend in part upon how long the cells have been stored before administration. In light of existing physiological data, we generally aim to keep hemoglobin concentrations greater than 9 g/dL during the first several days after TBI. In part, the decision is based on the patient's risk of or development of secondary ischemia or brain injury. An increasing number of centers use multimodal neurologic monitoring, which may help to individualize transfusion goals based on the degree of cerebral hypoxia or metabolic distress. When available, brain tissue oxygen tension values less than 15-20 mm Hg or a lactate:pyruvate ratio greater than 30-40 would influence us to use more aggressive hemoglobin correction (e.g., a transfusion threshold of 10 g/dL). Clinicians can attempt to reduce transfusion requirements by limiting phlebotomy, minimizing hemodilution, and providing appropriate prophylaxis against gastrointestinal hemorrhage. Administration of exogenous erythropoietin may have a small impact in further reducing the need for transfusion, but it also may increase complications, most notably deep venous thrombosis. Erythropoietin is currently of great interest as a potential neuroprotective agent, but until it is adequately evaluated in randomized controlled trials, it should not be used routinely for this purpose. HBBSs are also of interest, but existing preparations have not been shown to be beneficial-or even safe-in the context of TBI.
约50%的创伤性脑损伤(TBI)住院患者会发生贫血,贫血被认为是继发性脑损伤的一个原因。本综述通过文献检索研究贫血和输血对TBI患者的影响,以确定关于TBI中贫血和输血的原始研究、输血对脑生理学的影响以及促红细胞生成素或血红蛋白基血液替代品(HBBSs)的作用。然而,可用于帮助决定何时对TBI患者进行输血的高质量前瞻性数据非常少。随机输血试验涉及的TBI患者太少,无法得出明确结论。因此,广泛存在的实践差异也就不足为奇了。我们认为,对于入住医院尤其是重症监护病房(ICU)的TBI患者,7 g/dL的血红蛋白输血阈值尚不被认为是安全的,而对于其他重症患者则不然。红细胞输血通常对脑生理学有直接的、看似有益的影响,但这种影响的程度可能部分取决于细胞在输注前储存的时间。根据现有的生理学数据,我们通常旨在使TBI后的头几天血红蛋白浓度保持在9 g/dL以上。部分决策是基于患者发生继发性缺血或脑损伤的风险或情况。越来越多的中心使用多模式神经监测,这可能有助于根据脑缺氧或代谢窘迫程度个体化输血目标。当脑组织氧分压值低于15 - 20 mmHg或乳酸与丙酮酸比值大于30 - 40时,会促使我们采用更积极的血红蛋白纠正措施(例如,输血阈值为10 g/dL)。临床医生可以通过限制静脉穿刺、尽量减少血液稀释以及提供适当的胃肠道出血预防措施来尝试减少输血需求。给予外源性促红细胞生成素可能对进一步减少输血需求有较小影响,但也可能增加并发症,最显著的是深静脉血栓形成。促红细胞生成素作为一种潜在的神经保护剂目前备受关注,但在其在随机对照试验中得到充分评估之前,不应常规用于此目的。HBBSs也备受关注,但在TBI的情况下,现有的制剂尚未显示出有益甚至安全。
