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新生儿窒息的猪模型。

A swine model of neonatal asphyxia.

作者信息

Cheung Po-Yin, Gill Richdeep S, Bigam David L

机构信息

Departments of Pediatrics, Pharmacology and Surgery, University of Alberta.

出版信息

J Vis Exp. 2011 Oct 11(56):3166. doi: 10.3791/3166.

Abstract

Annually more than 1 million neonates die worldwide as related to asphyxia. Asphyxiated neonates commonly have multi-organ failure including hypotension, perfusion deficit, hypoxic-ischemic encephalopathy, pulmonary hypertension, vasculopathic enterocolitis, renal failure and thrombo-embolic complications. Animal models are developed to help us understand the patho-physiology and pharmacology of neonatal asphyxia. In comparison to rodents and newborn lambs, the newborn piglet has been proven to be a valuable model. The newborn piglet has several advantages including similar development as that of 36-38 weeks human fetus with comparable body systems, large body size (~1.5-2 kg at birth) that allows the instrumentation and monitoring of the animal and controls the confounding variables of hypoxia and hemodynamic derangements. We here describe an experimental protocol to simulate neonatal asphyxia and allow us to examine the systemic and regional hemodynamic changes during the asphyxiating and reoxygenation process as well as the respective effects of interventions. Further, the model has the advantage of studying multi-organ failure or dysfunction simultaneously and the interaction with various body systems. The experimental model is a non-survival procedure that involves the surgical instrumentation of newborn piglets (1-3 day-old and 1.5-2.5 kg weight, mixed breed) to allow the establishment of mechanical ventilation, vascular (arterial and central venous) access and the placement of catheters and flow probes (Transonic Inc.) for the continuously monitoring of intra-vascular pressure and blood flow across different arteries including main pulmonary, common carotid, superior mesenteric and left renal arteries. Using these surgically instrumented piglets, after stabilization for 30-60 minutes as defined by Z<10% variation in hemodynamic parameters and normal blood gases, we commence an experimental protocol of severe hypoxemia which is induced via normocapnic alveolar hypoxia. The piglet is ventilated with 10-15% oxygen by increasing the inhaled concentration of nitrogen gas for 2h, aiming for arterial oxygen saturations of 30-40%. This degree of hypoxemia will produce clinical asphyxia with severe metabolic acidosis, systemic hypotension and cardiogenic shock with hypoperfusion to vital organs. The hypoxia is followed by reoxygenation with 100% oxygen for 0.5 h and then 21% oxygen for 3.5 h. Pharmacologic interventions can be introduced in due course and their effects investigated in a blinded, block-randomized fashion.

摘要

全球每年有超过100万新生儿死于窒息相关原因。窒息新生儿通常会出现多器官功能衰竭,包括低血压、灌注不足、缺氧缺血性脑病、肺动脉高压、血管病变性小肠结肠炎、肾衰竭和血栓栓塞并发症。人们开发动物模型以帮助我们了解新生儿窒息的病理生理学和药理学。与啮齿动物和新生羔羊相比,新生仔猪已被证明是一种有价值的模型。新生仔猪有几个优点,包括其发育与36 - 38周的人类胎儿相似,身体系统具有可比性,体型较大(出生时约1.5 - 2千克),这便于对动物进行仪器安装和监测,并控制缺氧和血流动力学紊乱的混杂变量。我们在此描述一种实验方案,用于模拟新生儿窒息,并使我们能够检查窒息和复氧过程中的全身和区域血流动力学变化以及干预措施的各自效果。此外,该模型具有同时研究多器官功能衰竭或功能障碍以及与各种身体系统相互作用的优势。该实验模型是一种非存活程序,涉及对新生仔猪(1 - 3日龄,体重1.5 - 2.5千克,混合品种)进行外科手术仪器安装,以建立机械通气、血管(动脉和中心静脉)通路,并放置导管和流量探头(Transonic公司),用于连续监测不同动脉(包括主肺动脉、颈总动脉、肠系膜上动脉和左肾动脉)的血管内压力和血流。使用这些经过外科手术仪器安装的仔猪,在根据血流动力学参数变化<10%且血气正常定义的稳定30 - 60分钟后,我们开始通过常碳酸血症性肺泡缺氧诱导严重低氧血症的实验方案。通过增加氮气吸入浓度使仔猪以10 - 15%的氧气进行通气2小时,目标是动脉血氧饱和度达到30 - 40%。这种程度的低氧血症将导致临床窒息,伴有严重代谢性酸中毒、全身低血压和心源性休克以及对重要器官的灌注不足。低氧血症后用100%氧气复氧0.5小时,然后用21%氧气复氧3.5小时。可以在适当的时候引入药物干预措施,并以盲法、区组随机方式研究其效果。

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A swine model of neonatal asphyxia.新生儿窒息的猪模型。
J Vis Exp. 2011 Oct 11(56):3166. doi: 10.3791/3166.

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