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静脉注射全氟碳乳液 Oxycyte 不会增加非镇静猪模型中高压氧相关的癫痫发作。

The intravenous perfluorocarbon emulsion Oxycyte does not increase hyperbaric oxygen-related seizures in a non-sedated swine model.

机构信息

Undersea Medicine Department, Naval Medical Research Center, 503 Robert Grant Ave., Silver Spring, MD, 20910-7500, USA,

出版信息

Eur J Appl Physiol. 2013 Nov;113(11):2795-802. doi: 10.1007/s00421-013-2720-x. Epub 2013 Sep 6.

DOI:10.1007/s00421-013-2720-x
PMID:24062008
Abstract

PURPOSE

Standard treatment for decompression sickness (DCS) is recompression therapy with hyperbaric oxygen (HBO). Non-recompressive therapies are needed to address mass casualty scenarios such as a disabled submarine rescue or DCS therapy in remote environments. Intravenously delivered perfluorocarbon (PFC) emulsions improve blood oxygen content and decrease mortality in several animal models of DCS. However, the enhanced oxygen delivery of PFC emulsions may increase CNS oxygen toxicity (seizures) risk when used in conjunction with HBO. We studied seizure latency and duration in swine randomized to receive PFC or normal saline with 6 ATA of oxygen.

METHODS

Yorkshire swine (n = 31) were fitted with EEG electrodes and randomized to receive 5 ml/kg of the PFC Oxycyte (Oxygen Biotherapeutics Inc., Morrisville, NC) or saline intravenously 1 h before HBO. Unsedated animals were fitted with a snout mask for inhaled gas delivery, positioned inside the hyperbaric chamber, and compressed to 165 ft of sea water (6 ATA). After 2.5 min at 6 ATA, breathing gas was switched to 100 % O2 until signs of seizure were observed and EEG activity was evident. At seizure onset gas was switched back to air for 3 min, then the chamber was decompressed. After 24 h, the dive profile/oxygen exposure was repeated to ensure no secondary effects of PFC drug redistribution or emulsion metabolism.

RESULTS/CONCLUSION: Intravenous PFC emulsion did not decrease seizure latency or increase duration on initial HBO exposure or after 24 h. This finding demonstrates the safety of PFC use in conjunction with recompression therapy to treat DCS.

摘要

目的

减压病(DCS)的标准治疗方法是高压氧(HBO)再压缩治疗。在潜艇失能救援或偏远环境中的 DCS 治疗等大规模伤亡情况下,需要非再压缩治疗方法。静脉内给予全氟碳(PFC)乳液可改善几种 DCS 动物模型的血液氧含量并降低死亡率。然而,当与 HBO 一起使用时,PFC 乳液增强的氧输送可能会增加 CNS 氧毒性(癫痫发作)的风险。我们研究了接受 PFC 或 6 ATA 氧气生理盐水的猪的癫痫发作潜伏期和持续时间。

方法

给 31 头约克夏猪配备脑电图电极,并在 HBO 前 1 小时随机接受 5ml/kg 的 PFC Oxycyte(Oxygen Biotherapeutics Inc.,Morrisville,NC)或生理盐水静脉内给药。未镇静的动物佩戴鼻罩以输送吸入气体,置于高压舱内,并压缩至 165 英尺海水(6ATA)。在 6ATA 下 2.5 分钟后,呼吸气体切换为 100%氧气,直到观察到癫痫发作迹象和脑电图活动。在癫痫发作开始时,将气体切换回空气 3 分钟,然后减压。24 小时后,重复潜水剖面/氧气暴露以确保 PFC 药物重新分布或乳液代谢无二次影响。

结果/结论:静脉内 PFC 乳液在初始 HBO 暴露或 24 小时后均未降低癫痫发作潜伏期或延长持续时间。这一发现表明 PFC 与再压缩治疗联合使用治疗 DCS 的安全性。

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