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选择性脑灌注可改善体外心肺复苏后大鼠模型的神经结局。

Selective brain perfusion improves the neurological outcomes after extracorporeal cardiopulmonary resuscitation in a rat model.

机构信息

Cardiovascular Surgery, Department of Surgery, National Taiwan University Hospital and College of Medicine, Taipei, Taiwan.

Graduate Institute and Department of Physiology, College of Medicine, National Taiwan University, Taipei, Taiwan.

出版信息

Artif Organs. 2024 Jul;48(7):743-752. doi: 10.1111/aor.14732. Epub 2024 Feb 23.

Abstract

BACKGROUND

The major concern in patients who have suffered from cardiac arrest (CA) and undergone successful extracorporeal cardiopulmonary resuscitation (E-CPR) is poor neurological outcomes. In this study, we aimed to introduce a rat model of selective brain perfusion (SBP) during E-CPR to improve the neurological outcome after CA.

METHODS

The rats underwent 7 min of untreated asphyxial CA and then were resuscitated with E-CPR for 30 min. The right external jugular vein and right femoral artery were separately cannulated to the E-CPR outflow and inflow. The right common carotid artery was cannulated from the proximal to the distal side for SBP. Subsequently, rats were removed from E-CPR, wounds were closed, and 90 min of intensive care were provided. Neurological deficit scores were tested after 4 h of recovery when the rats were mechanical ventilation-free. S100 calcium-binding protein B (S100B) and glial fibrillary acidic protein (GFAP) were detected through immunohistochemistry (IHC) of brain tissue.

RESULTS

The rats that received SBP while resuscitated by E-CPR showed markedly better neurological performances after 4-h recovery than those resuscitated by E-CPR only. The IHC staining of GFAP and S100B in the hippocampus was low in the rats receiving SBP during E-CPR, but only GFAP showed significant differences.

CONCLUSIONS

We successfully developed a novel and reproducible rat model of SBP while resuscitated by E-CPR to ameliorate the neurological performances after CA. This achievement might have opportunities for studying how to improve the neurological outcome in the clinical condition.

摘要

背景

经历心脏骤停 (CA) 并成功接受体外心肺复苏术 (E-CPR) 的患者主要关注的是神经功能预后不良。在这项研究中,我们旨在引入 E-CPR 期间选择性脑灌注 (SBP) 的大鼠模型,以改善 CA 后的神经功能预后。

方法

大鼠经历 7 分钟未经处理的窒息性 CA,然后接受 E-CPR 复苏 30 分钟。右侧颈外静脉和右侧股动脉分别插管用于 E-CPR 的流出和流入。右侧颈总动脉从近端到远端插管进行 SBP。随后,大鼠从 E-CPR 中取出,关闭伤口,并提供 90 分钟的重症监护。在大鼠无需机械通气恢复 4 小时后进行神经功能缺损评分测试。通过脑组织免疫组织化学 (IHC) 检测 S100 钙结合蛋白 B (S100B) 和胶质纤维酸性蛋白 (GFAP)。

结果

接受 E-CPR 复苏时接受 SBP 的大鼠在 4 小时恢复后神经功能表现明显优于仅接受 E-CPR 复苏的大鼠。接受 E-CPR 时接受 SBP 的大鼠海马区 GFAP 和 S100B 的 IHC 染色较低,但只有 GFAP 有显著差异。

结论

我们成功开发了一种新的、可重复的 E-CPR 复苏时 SBP 的大鼠模型,以改善 CA 后的神经功能预后。这一成就可能为研究如何改善临床情况下的神经功能预后提供机会。

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