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Cerebral Microcirculation during Experimental Normovolaemic Anemia

机译:实验性非血液性贫血期间的脑微循环

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摘要

Anemia is accepted among critically ill patients as an alternative to elective blood transfusion. This practice has been extrapolated to head injury patients with only one study comparing the effects of mild anemia on neurological outcome. There are no studies quantifying microcirculation during anemia. Experimental studies suggest that anemia leads to cerebral hypoxia and increased rates of infarction, but the lack of clinical equipoise, when testing the cerebral effects of transfusion among critically injured patients, supports the need of experimental studies. The aim of this study was to quantify cerebral microcirculation and the potential presence of axonal damage in an experimental model exposed to normovolaemic anemia, with the intention of describing possible limitations within management practices in critically ill patients. Under non-recovered anesthesia, six Merino sheep were instrumented using an intracardiac transeptal catheter to inject coded microspheres into the left atrium to ensure systemic and non-chaotic distribution. Cytometric analyses quantified cerebral microcirculation at specific regions of the brain. Amyloid precursor protein staining was used as an indicator of axonal damage. Animals were exposed to normovolaemic anemia by blood extractions from the indwelling arterial catheter with simultaneous fluid replacement through a venous central catheter. Simultaneous data recording from cerebral tissue oxygenation, intracranial pressure, and cardiac output was monitored. A regression model was used to examine the effects of anemia on microcirculation with a mixed model to control for repeated measures. Homogeneous and normal cerebral microcirculation with no evidence of axonal damage was present in all cerebral regions, with no temporal variability, concluding that acute normovolaemic anemia does not result in short-term effects on cerebral microcirculation in the ovine brain.
机译:重症患者可以接受贫血作为选择性输血的替代方法。仅一项研究比较了轻度贫血对神经系统预后的影响,已将这种方法外推至头部受伤患者。尚无量化贫血期间微循环的研究。实验研究表明,贫血会导致脑缺氧并增加梗死发生率,但是,当在重症患者中测试输血对大脑的影响时,缺乏临床平衡就可以支持实验研究。这项研究的目的是在暴露于正常血液贫血症的实验模型中量化脑微循环和轴突损伤的潜在存在,目的是描述重症患者管理实践中的可能限制。在未恢复的麻醉下,使用心内穿入导管将六只美利奴羊植入仪器中,以将编码的微球体注入左心房,以确保全身性和非混沌性分布。细胞计数分析定量了大脑特定区域的大脑微循环。淀粉样前体蛋白染色被用作轴突损伤的指标。通过从留置动脉导管中抽血并同时通过静脉中央导管进行补液,使动物暴露于正常血红素性贫血。监测来自脑组织氧合,颅内压和心输出量的同时数据。使用回归模型来检查贫血对微循环的影响,并使用混合模型来控制重复测量。在所有脑区域均存在均质且正常的脑微循环,没有轴突损伤的证据,并且没有时间变化,因此得出结论,急性降血红细胞性贫血不会对绵羊脑内的脑微循环产生短期影响。

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