美金刚可改善脑片去极化扩散后的恢复情况,可考虑用于未来的临床试验。
Memantine Improves Recovery After Spreading Depolarization in Brain Slices and can be Considered for Future Clinical Trials.
机构信息
Department of Neurosciences, University of New Mexico School of Medicine, Albuquerque, NM, USA.
Department of Neurology, University of Utah School of Medicine, Salt Lake City, UT, USA.
出版信息
Neurocrit Care. 2021 Oct;35(Suppl 2):135-145. doi: 10.1007/s12028-021-01351-9. Epub 2021 Oct 17.
BACKGROUND
Spreading depolarization (SD) has been identified as a key mediator of secondary lesion progression after acute brain injuries, and clinical studies are beginning to pharmacologically target SDs. Although initial work has focused on the N-Methyl-D-aspartate receptor antagonist ketamine, there is also interest in alternatives that may be better tolerated. We recently showed that ketamine can inhibit mechanisms linked to deleterious consequences of SD in brain slices. The present study tested the hypothesis that memantine improves recovery of brain slices after SD and explored the effects of memantine in a clinical case targeting SD.
METHODS
For mechanistic studies, electrophysiological and optical recordings were made from hippocampal area CA1 in acutely prepared brain slices from mice. SDs were initiated by localized microinjection of K in conditions of either normal or reduced metabolic substrate availability. Memantine effects were assessed from intrinsic optical signals and extracellular potential recordings. For the clinical report, a subdural strip electrode was used for continuous electrocorticographic recording after the surgical evacuation of a chronic subdural hematoma.
RESULTS
In brain slice studies, memantine (10-300 µM) did not prevent the initiation of SD, but impaired SD propagation rate and recovery from SD. Memantine reduced direct current (DC) shift duration and improved recovery of synaptic potentials after SD. In brain slices with reduced metabolic substrate availability, memantine reduced the evidence of structural disruption after the passage of SD. In our clinical case, memantine did not noticeably immediately suppress SD; however, it was associated with a significant reduction of SD duration and a reduction in the electrocorticographic (ECoG) suppression that occurs after SD. SD was completely suppressed, with improvement in neurological examination with the addition of a brief course of ketamine.
CONCLUSIONS
These data extend recent work showing that N-Methyl-D-aspartate receptor antagonists can improve recovery from SD. These results suggest that memantine could be considered for future clinical trials targeting SD, and in some cases as an adjunct or alternative to ketamine.
背景
扩散性去极化(SD)已被确定为急性脑损伤后继发性损伤进展的关键介质,临床研究开始针对 SD 进行药理学靶向治疗。虽然最初的工作集中在 N-甲基-D-天冬氨酸受体拮抗剂氯胺酮上,但人们也对可能更耐受的替代药物感兴趣。我们最近表明,氯胺酮可以抑制脑片中与 SD 有害后果相关的机制。本研究检验了以下假设:美金刚可改善 SD 后脑片的恢复,并探索了美金刚在针对 SD 的临床病例中的作用。
方法
在急性制备的来自小鼠海马 CA1 区的脑片中进行电生理和光学记录,以进行机制研究。在正常或降低代谢底物可用性的条件下,通过局部微注射 K 引发 SD。从固有光学信号和细胞外电势记录评估美金刚的作用。对于临床报告,在慢性硬膜下血肿的手术清除后,使用硬膜下条带电极进行连续皮层脑电图记录。
结果
在脑片研究中,美金刚(10-300μM)不能预防 SD 的发生,但会损害 SD 的传播速度和 SD 后的恢复。美金刚减少了直流(DC)偏移持续时间,并改善了 SD 后的突触电位恢复。在代谢底物可用性降低的脑片中,美金刚减少了 SD 通过后的结构破坏的证据。在我们的临床病例中,美金刚并没有立即明显抑制 SD;然而,它与 SD 持续时间的显著减少以及 SD 后发生的脑电图(ECoG)抑制的减少有关。SD 完全被抑制,在添加短暂的氯胺酮疗程后,神经检查得到改善。
结论
这些数据扩展了最近的研究结果,表明 N-甲基-D-天冬氨酸受体拮抗剂可以改善 SD 的恢复。这些结果表明,美金刚可考虑用于针对 SD 的未来临床试验,在某些情况下可作为氯胺酮的辅助或替代药物。
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