首页> 外文期刊>Journal of Cerebral Blood Flow and Metabolism: Official Journal of the International Society of Cerebral Blood Flow and Metabolism >Perinatal hypoxic-ischemic brain injury in large animal models: Relevance to human neonatal encephalopathy
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Perinatal hypoxic-ischemic brain injury in large animal models: Relevance to human neonatal encephalopathy

机译:大型动物模型中围产期缺氧缺血性脑损伤:与人类新生儿脑病的相关性

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摘要

Perinatal hypoxia-ischemia resulting in death or lifelong disabilities remains a major clinical disorder. Neonatal models of hypoxia-ischemia in rodents have enhanced our understanding of cellular mechanisms of neural injury in developing brain, but have limitations in simulating the range, accuracy, and physiology of clinical hypoxia-ischemia and the relevant systems neuropathology that contribute to the human brain injury pattern. Large animal models of perinatal hypoxia-ischemia, such as partial or complete asphyxia at the time of delivery of fetal monkeys, umbilical cord occlusion and cerebral hypoperfusion at different stages of gestation in fetal sheep, and severe hypoxia and hypoperfusion in newborn piglets, have largely overcome these limitations. In monkey, complete asphyxia produces preferential injury to cerebellum and primary sensory nuclei in brainstem and thalamus, whereas partial asphyxia produces preferential injury to somatosensory and motor cortex, basal ganglia, and thalamus. Mid-gestational fetal sheep provide a valuable model for studying vulnerability of progenitor oligodendrocytes. Hypoxia followed by asphyxia in newborn piglets replicates the systems injury seen in term newborns. Efficacy of post-insult hypothermia in animal models led to the success of clinical trials in term human neonates. Large animal models are now being used to explore adjunct therapy to augment hypothermic neuroprotection.
机译:导致死亡或终身残疾导致死亡或终身残疾的围产期缺血仍然是一个重大的临床疾病。啮齿动物中缺氧缺血的新生儿模型提高了我们对发展大脑神经损伤细胞机制的理解,但在模拟临床缺氧缺血和相关系统神经病理学的范围,准确性和生理学方面具有局限性的局限性伤害模式。围产期缺氧缺血的大型动物模型,如胎儿猴子递送时的部分或完全窒息,在胎儿羊的不同阶段的不同阶段,并且在新生仔猪中的严重缺氧和低血量繁殖时,具有很大程度上克服这些限制。在猴子中,完全窒息在脑干和丘脑中产生优先损伤,而脑干和丘脑的主要感觉核产生优先损伤,而部分窒息会对躯体感应和电机皮质,基础神经节和丘脑产生优先损伤。中妊娠胎儿绵羊为研究祖先少突胶质细胞的脆弱性提供了有价值的模型。缺氧随后是新生仔猪中的窒息复制了新生儿术语中看到的系统损伤。侮辱后体温过低在动物模型中的疗效导致临床试验在人类新生儿中的成功。现在正在使用大型动物模型来探索辅助治疗以增加低温神经保护作用。

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