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空间 T 迷宫在海马锥体神经元丢失和中间神经元减少的模型中,可识别缺氧缺血后 1 个月仔猪的认知缺陷。

Spatial T-maze identifies cognitive deficits in piglets 1 month after hypoxia-ischemia in a model of hippocampal pyramidal neuron loss and interneuron attrition.

机构信息

Johns Hopkins University (JHU), Department of Anesthesiology and Critical Care Medicine, Baltimore, MD, United States.

JHU Department of Pathology, Baltimore, MD, United States.

出版信息

Behav Brain Res. 2019 Sep 2;369:111921. doi: 10.1016/j.bbr.2019.111921. Epub 2019 Apr 19.

Abstract

Neonatal brain injury from hypoxia-ischemia (HI) causes major morbidity. Piglet HI is an established method for testing neuroprotective treatments in large, gyrencephalic brain. Though many neurobehavior tests exist for rodents, such tests and their associations with neuropathologic injury remain underdeveloped and underutilized in large, neonatal HI animal models. We examined whether spatial T-maze and inclined beam tests distinguish cognitive and motor differences between HI and sham piglets and correlate with neuropathologic injury. Neonatal piglets were randomized to whole-body HI or sham procedure, and they began T-maze and inclined beam testing 17 days later. HI piglets had more incorrect T-maze turns than did shams. Beam walking time did not differ between groups. Neuropathologic evaluations at 33 days validated the injury with putamen neuron loss after HI to below that of sham procedure. HI decreased the numbers of CA3 pyramidal neurons but not CA1 pyramidal neurons or dentate gyrus granule neurons. Though the number of hippocampal parvalbumin-positive interneurons did not differ between groups, HI reduced the number of CA1 interneuron dendrites. Piglets with more incorrect turns had greater CA3 neuron loss, and piglets that took longer in the maze had fewer CA3 interneurons. The number of putamen neurons was unrelated to T-maze or beam performance. We conclude that neonatal HI causes hippocampal CA3 neuron loss, CA1 interneuron dendritic attrition, and putamen neuron loss at 1-month recovery. The spatial T-maze identifies learning and memory deficits that are related to loss of CA3 pyramidal neurons and fewer parvalbumin-positive interneurons independent of putamen injury.

摘要

缺氧缺血性(HI)新生儿脑损伤会导致重大发病率。猪仔 HI 是测试大型脑回状大脑中神经保护治疗的既定方法。虽然啮齿动物有许多神经行为测试,但这些测试及其与神经病理学损伤的关联在大型新生 HI 动物模型中仍未得到充分发展和利用。我们研究了空间 T 迷宫和倾斜梁测试是否能区分 HI 和假手术仔猪的认知和运动差异,并与神经病理学损伤相关。新生仔猪随机分为全身 HI 或假手术组,然后在 17 天后开始 T 迷宫和倾斜梁测试。HI 仔猪比假手术仔猪在 T 迷宫中有更多的错误转弯。两组之间的横梁行走时间没有差异。33 天时的神经病理学评估验证了 HI 导致纹状体神经元丢失,低于假手术组。HI 减少了 CA3 锥体神经元的数量,但不减少 CA1 锥体神经元或齿状回颗粒神经元的数量。尽管两组之间的海马 CA1 神经元树突数量没有差异,但 HI 减少了 CA1 中间神经元的树突数量。转弯错误较多的仔猪 CA3 神经元丢失较多,迷宫中花费时间较长的仔猪 CA3 中间神经元较少。纹状体神经元数量与 T 迷宫或横梁性能无关。我们的结论是,新生 HI 导致海马 CA3 神经元丢失、CA1 中间神经元树突萎缩和 1 个月恢复期纹状体神经元丢失。空间 T 迷宫可识别学习和记忆缺陷,与 CA3 锥体神经元丢失和较少的 parvalbumin 阳性中间神经元有关,与纹状体损伤无关。

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