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早期新生大鼠注射192IgG皂草素会导致学习障碍并扰乱其皮质形态发生。

Early neonatal 192 IgG saporin induces learning impairments and disrupts cortical morphogenesis in rats.

作者信息

Ricceri Laura, Hohmann Christine, Berger-Sweeney Joanne

机构信息

Section of Comparative Psychology, Laboratory Fisiopatologia OS, Istituto Superiore di Sanità, Vle Regina Elena 299, I-00161 Rome, Italy.

出版信息

Brain Res. 2002 Nov 8;954(2):160-72. doi: 10.1016/s0006-8993(02)03172-4.

Abstract

We have shown previously that neonatal intraventricular injections of the selective cholinergic immunotoxin 192 IgG saporin on postnatal day 7 (pnd 7) induce marked cholinergic loss in hippocampus and neocortex and a learning impairment on pnd 15. In the present study, we analysed the behavioural, morphological and neurochemical effects of earlier intraventricular injection of the immunotoxin 192 IgG saporin (pnd 1 and 3). We hypothesised that these earlier lesions would interrupt a critical stage in neocortical maturation, and impair behavior more profoundly than the later lesions. Passive avoidance (PA) learning and locomotor activity during the PA test were assessed on pnd 15. Retention of the PA task was assessed on pnd 16. Reactivity to spatial and object novelty was assessed on pnd 180 in a spatial open field test with five objects. Choline acetyltransferase (ChAT) activity was measured in basal forebrain targets on pnd 20 and pnd 180. Neonatal administration of 192 IgG saporin resulted in a slower acquisition of the PA task in females; retention and locomotor activity were not affected. On pnd 180, reaction to spatial novelty was mildly impaired in lesioned rats of both sexes. There was a marked reduction of ChAT in the hippocampus and neocortex of lesioned rats of both sexes, at both ages. Morphological analysis of the somatosensory cortex of lesioned rats revealed alterations in cortical development with sex specific variations in total cortical thickness. These results suggest that interrupting cholinergic basal forebrain innervation of neocortex and hippocampus during the first postnatal days affects the development of cognitive behaviour, neurochemistry and cortical organisation in a sex specific manner. Furthermore, the alterations in cortical organization are more profound than those noted after a lesion later in postnatal development. These behavioural and morphological abnormalities could be considered a model for several neurodevelopmental disorders associated with mental retardation.

摘要

我们之前已经表明,在出生后第7天(pnd 7)对新生大鼠进行脑室内注射选择性胆碱能免疫毒素192 IgG皂草素,会导致海马体和新皮质中明显的胆碱能丧失,并在pnd 15时出现学习障碍。在本研究中,我们分析了更早进行脑室内注射免疫毒素192 IgG皂草素(pnd 1和3)的行为、形态学和神经化学效应。我们假设这些早期损伤会中断新皮质成熟的关键阶段,并比后期损伤更严重地损害行为。在pnd 15评估被动回避(PA)学习和PA测试期间的运动活动。在pnd 16评估PA任务的保持情况。在pnd 180,通过一个有五个物体的空间旷场试验评估对空间和物体新奇性的反应性。在pnd 20和pnd 180测量基底前脑靶点中的胆碱乙酰转移酶(ChAT)活性。新生大鼠给予192 IgG皂草素后,雌性大鼠在PA任务的习得方面较慢;保持情况和运动活动未受影响。在pnd 180,两性受损伤大鼠对空间新奇性的反应均有轻度受损。在两个年龄段,两性受损伤大鼠的海马体和新皮质中的ChAT均显著减少。对受损伤大鼠体感皮质的形态学分析显示皮质发育存在改变,且总皮质厚度存在性别特异性差异。这些结果表明,在出生后的头几天中断新皮质和海马体的胆碱能基底前脑神经支配,会以性别特异性方式影响认知行为、神经化学和皮质组织的发育。此外,皮质组织的改变比出生后发育后期损伤后所观察到的更为严重。这些行为和形态学异常可被视为与智力迟钝相关的几种神经发育障碍的模型。

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