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Blood Brain Barrier is Impermeable to Solutes and Permeable to Waterafter Experimental Pediatric Cardiac Arrest

机译:血脑屏障对溶质不渗透对水不渗透实验性小儿心脏骤停后

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摘要

Pediatric asphyxial cardiac arrest (CA) results in unfavorable neurological outcome in most survivors. Development of neuroprotective therapies is contingent upon understanding the permeability of intravenously delivered medications through the blood brain barrier (BBB). In a model of pediatric CA we sought to characterize BBB permeability to small and large molecular weight substances. Additionally, we measured the percent brain water after CA.Asphyxia of 9 min was induced in 16-18 day-old rats. The rats were resuscitated and the BBB permeability to small (sodium fluorescein and gadoteridol) and large (immunoglobulin G, IgG) molecules was assessed at 1, 4, and 24 h after asphyxial CA or sham surgery. Percent brain water was measured post-CA and in shams using wet-to-dry brain weight.Fluorescence, gadoteridol uptake, or IgG staining at 1, 4 h and over the entire 24 h post-CA did not differ from shams, suggesting absence of BBB permeability to these solutes. Cerebral water content was increased at 3 h post-CA vs. sham.In conclusion, after 9 min of asphyxial CA there is no BBB permeability over 24 h to conventional small or large molecule tracers despite the fact that cerebral water content is increased early post-CA indicating the development of brain edema. Evaluation of novel therapies targeting neuronal death after pediatric CA should include their capacity to cross the BBB.
机译:小儿窒息性心脏骤停(CA)在大多数幸存者中导致不良的神经系统预后。神经保护疗法的发展取决于了解静脉注射药物通过血脑屏障(BBB)的渗透性。在儿科CA模型中,我们试图表征BBB对小分子量和大分子量物质的渗透性。另外,我们测量了CA后脑水的百分比。在16-18日龄的大鼠中诱导了9分钟的窒息。复苏大鼠,并在窒​​息性CA或假手术后1、4和24小时评估BBB对小分子(荧光素钠和gadoteridol)和大分子(免疫球蛋白G,IgG)的通透性。在CA后和干毛干中使用干重来测量脑水百分比.CA后1,4 h以及整个24小时的荧光,gadoteridol摄取或IgG染色与毛干无差异,表明缺乏BBB对这些溶质的渗透性。与假手术相比,CA后3小时脑水含量增加。总的来说,窒息CA 9分钟后,传统的小分子或大分子示踪剂在24小时内都没有BBB渗透性,尽管脑水含量在术后早期增加-CA表示脑水肿的发展。小儿CA后针对神经元死亡的新型疗法的评估应包括其穿越血脑屏障的能力。

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