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冷却联合即刻或延迟氙气吸入在新生儿缺氧缺血后提供同等的长期神经保护作用。

Cooling combined with immediate or delayed xenon inhalation provides equivalent long-term neuroprotection after neonatal hypoxia-ischemia.

作者信息

Thoresen Marianne, Hobbs Catherine E, Wood Tommy, Chakkarapani Ela, Dingley John

机构信息

Department of Clinical Sciences at South Bristol, University of Bristol, Bristol, UK.

出版信息

J Cereb Blood Flow Metab. 2009 Apr;29(4):707-14. doi: 10.1038/jcbfm.2008.163. Epub 2009 Jan 14.

DOI:10.1038/jcbfm.2008.163
PMID:19142190
Abstract

Hypothermia (HT) improves outcome after neonatal hypoxia-ischemia. Combination therapy may extend neuroprotection. The noble anesthetic gas xenon (Xe) has an excellent safety profile. We have shown earlier that 3 h of 50% Xe plus HT (32 degrees C) additively gives more protection (72%) than either alone (HT=31.1%, Xe=10.2%). Factors limiting clinical use include high-cost and specialist administration requirements. Thus, combinations of 1 h of 50% Xe were administered concurrently for either the first (1 h(Immediate)Xe) or last (1 h(Delayed)Xe) of 3 h of posthypoxic-ischemic HT as compared with 3 h of 50%Xe/HT to investigate how brief Xe exposure with a delay would affect efficacy. An established neonatal rat hypoxia-ischemia model was used. Serial functional neurologic testing into adulthood was performed, followed by neuropathological examination. Xenon with HT was more effective with longer Xe duration (3 h versus 1 h) (P=0.015). However, 1 h Xe/3 h HT resulted in better neuroprotection than 3 h HT alone (P=0.03), this significant effect was also present with 1 h Xe after a 2-h delay. One (immediate or with a delay) or 3 h Xe also significantly improved motor function (P=0.024). Females had significantly better motor scores than males, but no sex-dependent difference in pathology results. The neuroprotection of short, delayed Xe treatment would allow transport to specialist facilities to receive Xe.

摘要

低温疗法(HT)可改善新生儿缺氧缺血后的预后。联合治疗可能会延长神经保护作用。惰性麻醉气体氙气(Xe)具有出色的安全性。我们之前已经表明,50%氙气加HT(32摄氏度)持续3小时的联合治疗比单独使用任何一种疗法(HT = 31.1%,Xe = 10.2%)具有更强的保护作用(72%)。限制其临床应用的因素包括成本高和需要专业人员管理。因此,与50%氙气/HT持续3小时相比,在缺氧缺血后HT的3小时治疗中,分别在开始的1小时(即刻1小时Xe)或最后的1小时(延迟1小时Xe)同时给予1小时50%氙气,以研究延迟的短暂氙气暴露会如何影响疗效。使用已建立的新生大鼠缺氧缺血模型。对成年后的大鼠进行系列功能性神经测试,随后进行神经病理学检查。氙气与HT联合使用时,氙气持续时间较长(3小时与1小时)时效果更佳(P = 0.015)。然而,1小时Xe/3小时HT比单独3小时HT具有更好的神经保护作用(P = 0.03),在延迟2小时后给予1小时Xe时也存在这种显著效果。1小时(即刻或延迟)或3小时Xe也显著改善了运动功能(P = 0.024)。雌性大鼠的运动评分明显高于雄性,但病理结果不存在性别依赖性差异。短暂、延迟的Xe治疗的神经保护作用将允许将动物转运至专业机构接受Xe治疗。

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