International Experimental Central Nervous System Injury & Repair (IECNSIR), Department of Surgical Sciences, Anesthesiology & Intensive Care Medicine, Uppsala University Hospital, Uppsala University, Uppsala, Sweden.
Department of Clinical Neurosciences, University of Medicine & Pharmacy, Cluj-Napoca, Romania; "RoNeuro" Institute for Neurological Research and Diagnostic, Cluj-Napoca, Romania.
Int Rev Neurobiol. 2019;146:45-81. doi: 10.1016/bs.irn.2019.06.006. Epub 2019 Jul 8.
Several lines of evidences show that anesthetics influence neurotoxicity and neuroprotection. The possibility that different anesthetic agents potentially influence the pathophysiological and functional outcome following neurotrauma was examined in a rat model of concussive head injury (CHI). The CHI was produced by an impact of 0.224N on the right parietal bone by dropping a weight of 114.6g from a 20cm height under different anesthetic agents, e.g., inhaled ether anesthesia or intraperitoneally administered ketamine, pentobarbital, equithesin or urethane anesthesia. Five hour CHI resulted in profound volume swelling and brain edema formation in both hemispheres showing disruption of the blood-brain barrier (BBB) to Evans blue and radioiodine. A marked decrease in the cortical CBF and a profound increase in plasma or brain serotonin levels were seen at this time. Neuronal damages were present in several parts of the brain. These pathological changes were most marked in CHI under ether anesthesia followed by ketamine (35mg/kg, i.p.), pentobarbital (50mg/kg, i.p.), equithesin (3mL/kg, i.p.) and urethane (1g/kg, i.p.). The functional outcome on Rota Rod performances or grid walking tests was also most adversely affected after CHI under ether anesthesia followed by pentobarbital, equithesin and ketamine. Interestingly, the plasma and brain serotonin levels strongly correlated with the development of brain edema in head injured animals in relation to different anesthetic agents used. These observations suggest that anesthetic agents are detrimental to functional and pathological outcomes in CHI probably through influencing the circulating plasma and brain serotonin levels, not reported earlier. Whether anesthetics could also affect the efficacy of different neuroprotective agents in CNS injuries is a new subject that is currently being examined in our laboratory.
有几条证据表明,麻醉剂会影响神经毒性和神经保护作用。在撞击性颅脑损伤(CHI)的大鼠模型中,研究了不同麻醉剂是否会影响神经外伤后的病理生理和功能结果。通过从 20 厘米的高度将 114.6 克的重物落在右侧顶骨上,产生 CHI,在不同的麻醉剂下,如吸入乙醚麻醉或腹膜内给予氯胺酮、戊巴比妥、安乐酮或尿烷麻醉。5 小时的 CHI 导致双侧半球明显的体积肿胀和脑水肿形成,显示血脑屏障(BBB)对伊文思蓝和放射性碘的破坏。此时,皮质 CBF 明显下降,血浆或脑 5-羟色胺水平显著升高。大脑的几个部位存在神经元损伤。这些病理变化在乙醚麻醉下的 CHI 中最为明显,其次是氯胺酮(35mg/kg,ip)、戊巴比妥(50mg/kg,ip)、安乐酮(3mL/kg,ip)和尿烷(1g/kg,ip)。在乙醚麻醉下的 CHI 后,Rota Rod 性能或网格行走测试的功能结果也受到最不利的影响,其次是戊巴比妥、安乐酮和氯胺酮。有趣的是,血浆和脑 5-羟色胺水平与不同麻醉剂相关的颅脑损伤动物脑水肿的发展密切相关。这些观察结果表明,麻醉剂可能通过影响循环血浆和脑 5-羟色胺水平,对 CHI 的功能和病理结果产生不利影响,这在以前的报道中尚未提及。麻醉剂是否也会影响中枢神经系统损伤中不同神经保护剂的疗效,是目前我们实验室正在研究的一个新课题。
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