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小鼠对新生期基底前脑损伤的性别二态性反应:II. 皮质形态学

Sexually dimorphic responses to neonatal basal forebrain lesions in mice: II. Cortical morphology.

作者信息

Hohmann C F, Berger-Sweeney J

机构信息

Department of Biology, Morgan State University, Baltimore, Maryland 21215, USA.

出版信息

J Neurobiol. 1998 Dec;37(4):595-606.

PMID:9858261
Abstract

Previous studies in the mouse have shown that neonatal lesions to the cholinergic basal forebrain (nBM) areas result in transient cholinergic depletion of neocortex and precipitate altered cortical morphogenesis. Lesion-induced morphological alterations in cortex persist into adulthood and are accompanied by behavioral changes, including spatial memory deficits. The current study investigated whether neonatal nBM lesions affect male and female mice differently in adulthood. Quantitative morphometry of cortical layer width was employed to assess alterations in cytoarchitecture in neonatally nBM-lesioned and littermate control mice of both sexes following behavioral testing. Our results showed significant decreases in cortical layer IV and V widths across somato/motor cortex in neonatally nBM lesioned mice of both sexes. Sexually dimorphic responses were observed in cortical layer II/III and total cortical width, limited to the area containing the "barrel cortex" representation of the whisker hairs. In lesioned females, layer II/III and total cortical width were decreased relative to female controls, and in lesioned males, layer II/III was increased relative to controls, whereas total cortical width was unchanged. In male but not female mice we observed significant correlations between decreased widths in layer IV and V and impaired performance on a spatial memory task. The current data further support a role of developing cholinergic cortical afferents in the modulation of cortical morphogenesis and cortical circuits involved in cognitive behaviors. In addition, our observations provide further evidence for sexually dimorphic development and function in cognitive centers of the rodent brain.

摘要

先前对小鼠的研究表明,新生儿期胆碱能基底前脑(nBM)区域受损会导致新皮质的胆碱能暂时耗竭,并促使皮质形态发生改变。损伤诱导的皮质形态学改变会持续到成年期,并伴有行为变化,包括空间记忆缺陷。本研究调查了新生儿期nBM损伤对成年雄性和雌性小鼠的影响是否不同。在行为测试后,采用皮质层宽度的定量形态学方法评估了新生期nBM损伤的雌雄小鼠及同窝对照小鼠的细胞结构变化。我们的结果显示,新生期nBM损伤的雌雄小鼠躯体感觉/运动皮质的IV层和V层宽度均显著降低。在皮质II/III层和总皮质宽度上观察到了性别差异反应,且仅限于包含胡须“桶状皮质”表征的区域。在损伤的雌性小鼠中,II/III层和总皮质宽度相对于雌性对照降低;在损伤的雄性小鼠中,II/III层相对于对照增加,而总皮质宽度不变。在雄性而非雌性小鼠中,我们观察到IV层和V层宽度的降低与空间记忆任务表现受损之间存在显著相关性。目前的数据进一步支持了发育中的胆碱能皮质传入神经在调节皮质形态发生和参与认知行为的皮质回路中的作用。此外,我们的观察结果为啮齿动物大脑认知中心的性别差异发育和功能提供了进一步的证据。

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