Dai Xingping, Bragina Olga, Zhang Tongsheng, Yang Yirong, Rao Gutti R, Bragin Denis E, Statom Gloria, Nemoto Edwin M
1Integrated Traditional Chinese and Western Medicine, Xiangya Hospital, Central South University, Changsha, China. 2Department of Neurosurgery, University of New Mexico, Albuquerque, NM. 3Department of Pharmaceutical Sciences, BRaIN Imaging Center, College of Pharmacy, University of New Mexico, Albuquerque, NM. 4Department of Pathology and Laboratory Medicine, VA Pittsburgh Health Care System, Pittsburgh, PA.
Crit Care Med. 2016 Aug;44(8):e633-8. doi: 10.1097/CCM.0000000000001625.
We recently showed that increased intracranial pressure to 50 mm Hg in the healthy rat brain results in microvascular shunt flow characterized by tissue hypoxia, edema, and increased blood-brain barrier permeability. We now determined whether increased intracranial pressure results in neuronal injury by Fluoro-Jade stain and whether changes in cerebral blood flow and cerebral metabolic rate for oxygen suggest nonnutritive microvascular shunt flow.
Intracranial pressure was elevated by a reservoir of artificial cerebrospinal fluid connected to the cisterna magna. Arterial blood gases, cerebral arterial-venous oxygen content difference, and cerebral blood flow by MRI were measured. Fluoro-Jade stain neurons were counted in histologic sections of the right and left dorsal and lateral cortices and hippocampus.
University laboratory.
Male Sprague Dawley rats.
Arterial pressure support if needed by IV dopamine infusion and base deficit corrected by sodium bicarbonate.
Fluoro-Jade stain neurons increased 2.5- and 5.5-fold at intracranial pressures of 30 and 50 mm Hg and cerebral perfusion pressures of 57 ± 4 (mean ± SEM) and 47 ± 6 mm Hg, respectively (p < 0.001) (highest in the right and left cortices). Voxel frequency histograms of cerebral blood flow showed a pattern consistent with microvascular shunt flow by dispersion to higher cerebral blood flow at high intracranial pressure and decreased cerebral metabolic rate for oxygen.
High intracranial pressure likely caused neuronal injury because of a transition from normal capillary flow to nonnutritive microvascular shunt flow resulting in tissue hypoxia and edema, and it is manifest by a reduction in the cerebral metabolic rate for oxygen.
我们最近发现,健康大鼠脑内颅内压升高至50 mmHg会导致微血管分流,其特征为组织缺氧、水肿以及血脑屏障通透性增加。我们现在确定颅内压升高是否会通过氟玉染色导致神经元损伤,以及脑血流量和脑氧代谢率的变化是否提示存在非营养性微血管分流。
通过连接至枕大池的人工脑脊液储液器升高颅内压。测量动脉血气、脑动静脉氧含量差以及通过MRI测量脑血流量。对左右背侧和外侧皮质以及海马的组织切片中的氟玉染色神经元进行计数。
大学实验室。
雄性Sprague Dawley大鼠。
必要时通过静脉输注多巴胺支持动脉压,并用碳酸氢钠纠正碱缺失。
在颅内压分别为30和50 mmHg、脑灌注压分别为57±4(均值±标准误)和47±6 mmHg时,氟玉染色神经元分别增加了2.5倍和5.5倍(p<0.001)(在左右皮质中最高)。脑血流量的体素频率直方图显示出一种模式,与高颅内压时向更高脑血流量的弥散以及脑氧代谢率降低导致的微血管分流一致。
高颅内压可能由于从正常毛细血管血流转变为非营养性微血管分流,导致组织缺氧和水肿,从而引起神经元损伤,其表现为脑氧代谢率降低。