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严重围产期缺氧缺血性脑损伤以性别、年龄和任务选择性方式在C57BL/6小鼠中诱发长期感觉运动缺陷、焦虑样行为和认知障碍,但可通过新生儿期护理进行调节。

Severe Perinatal Hypoxic-Ischemic Brain Injury Induces Long-Term Sensorimotor Deficits, Anxiety-Like Behaviors and Cognitive Impairment in a Sex-, Age- and Task-Selective Manner in C57BL/6 Mice but Can Be Modulated by Neonatal Handling.

作者信息

Muntsant Aida, Shrivastava Kalpana, Recasens Mireia, Giménez-Llort Lydia

机构信息

Department of Psychiatry and Forensic Medicine, School of Medicine, Universitat Autònoma de Barcelona, Barcelona, Spain.

Institut de Neurociències, Universitat Autònoma de Barcelona, Barcelona, Spain.

出版信息

Front Behav Neurosci. 2019 Feb 13;13:7. doi: 10.3389/fnbeh.2019.00007. eCollection 2019.

Abstract

Perinatal brain injury (PBI) leads to neurological disabilities throughout life, from motor deficits, cognitive limitations to severe cerebral palsy. Yet, perinatal brain damage has limited therapeutic outcomes. Besides, the immature brain of premature children is at increased risk of hypoxic/ischemic (HI) injury, with males being more susceptible to it and less responsive to protective/therapeutical interventions. Here, we model in male and female C57BL/6 mice, the impact of neonatal HI and the protective effects of neonatal handling (NH), an early life tactile and proprioceptive sensory stimulation. From postnatal day 1 (PND1, modeling pre-term) to PND21 randomized litters received either NH or left undisturbed. HI brain damage occurred by permanent left carotid occlusion followed by hypoxia at PND7 (modeling full-term) in half of the animals. The behavioral and functional screening of the pups at weaning (PND23) and their long-term outcomes (adulthood, PND70) were evaluated in a longitudinal study, as follows: somatic development (weight), sensorimotor functions (reflexes, rods and hanger tests), exploration [activity (ACT) and open-field (OF) test], emotional and anxiety-like behaviors [corner, open-field and dark-light box (DLB) tests], learning and memory [T-maze (TM) and Morris Water-Maze (MWM)]. HI induced similar brain damage in both sexes but affected motor development, sensorimotor functions, induced hyperactivity at weaning, and anxiety-like behaviors and cognitive deficits at adulthood, in a sex- and age-dependent manner. Thus, during ontogeny, HI affected equilibrium especially in females and prehensility in males, but only reflexes at adulthood. Hyperactivity of HI males was normalized at adulthood. HI increased neophobia and other anxiety-like behaviors in males but emotionality in females. Both sexes showed worse short/long-term learning, but memory was more affected in males. Striking neuroprotective effects of NH were found, with significantly lower injury scores, mostly in HI males. At the functional level, NH reversed the impaired reflex responses and improved memory performances in hippocampal-dependent spatial-learning tasks, especially in males. Finally, neuropathological correlates referred to atrophy, neuronal densities and cellularity in the affected areas [hippocampal-CA, caudate/putamen, thalamus, neocortex and corpus callosum (CC)] point out distinct neuronal substrates underlying the sex- and age- functional impacts of these risk/protection interventions on sensorimotor, behavioral and cognitive outcomes from ontogeny to adulthood.

摘要

围产期脑损伤(PBI)会导致终身神经功能障碍,从运动缺陷、认知局限到严重的脑瘫。然而,围产期脑损伤的治疗效果有限。此外,早产儿未成熟的大脑发生缺氧缺血(HI)损伤的风险增加,男性更容易受到影响,且对保护性/治疗性干预的反应较差。在此,我们以雄性和雌性C57BL/6小鼠为模型,研究新生儿HI的影响以及新生儿抚触(NH)的保护作用,NH是一种早期的触觉和本体感觉刺激。从出生后第1天(PND1,模拟早产)到PND21,将随机分组的幼崽分为接受NH组或不进行干预组。在一半的动物中,于PND7时通过永久性左侧颈总动脉闭塞并随后缺氧来造成HI脑损伤(模拟足月)。在一项纵向研究中,对幼崽在断奶时(PND23)及其长期结局(成年期,PND70)进行行为和功能筛查,具体如下:躯体发育(体重)、感觉运动功能(反射、棒和悬挂测试)、探索行为[活动(ACT)和旷场(OF)测试]、情绪和焦虑样行为[角落、旷场和明暗箱(DLB)测试]、学习和记忆[T迷宫(TM)和莫里斯水迷宫(MWM)]。HI在两性中均导致类似的脑损伤,但以性别和年龄依赖性方式影响运动发育、感觉运动功能,在断奶时诱发多动,在成年期诱发焦虑样行为和认知缺陷。因此,在个体发育过程中,HI影响平衡,尤其是对雌性而言,影响抓握能力,尤其是对雄性而言,但仅在成年期影响反射。HI雄性在成年期的多动症状得到缓解。HI增加了雄性的新事物恐惧和其他焦虑样行为,但增加了雌性的情绪反应。两性在短期/长期学习方面均表现较差,但记忆在雄性中受影响更大。发现NH具有显著的神经保护作用,损伤评分显著降低,主要见于HI雄性。在功能水平上,NH逆转了受损的反射反应,并改善了海马依赖性空间学习任务中的记忆表现,尤其是在雄性中。最后,神经病理学相关性研究涉及受影响区域[海马体-CA、尾状核/壳核、丘脑、新皮层和胼胝体(CC)]的萎缩、神经元密度和细胞数量,指出了这些风险/保护干预措施对从个体发育到成年期的感觉运动、行为和认知结局产生性别和年龄依赖性功能影响的不同神经元基质。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/fbdc/6381068/02ce37da2235/fnbeh-13-00007-g0001.jpg

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