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前额叶和小脑小白蛋白神经元数量的改变与雄性大鼠的认知变化有关。

Altered prefrontal and cerebellar parvalbumin neuron counts are associated with cognitive changes in male rats.

作者信息

King Cole, Maze Tessa, Plakke Bethany

机构信息

Psychological Sciences, Kansas State University, 1114 Mid-Campus Dr., Manhattan, KS, 66506, USA.

出版信息

Exp Brain Res. 2024 Oct;242(10):2295-2308. doi: 10.1007/s00221-024-06902-y. Epub 2024 Jul 31.

Abstract

Exposure to valproic acid (VPA), a common anti-seizure medication, in utero is a risk factor for autism spectrum disorder (ASD). People with ASD often display changes in the cerebellum, including volume changes, altered circuitry, and changes in Purkinje cell populations. ASD is also characterized by changes in the medial prefrontal cortex (mPFC), where excitatory/inhibitory balance is often altered. This study exposed rats to a high dose of VPA during gestation and assessed cognition and anxiety-like behaviors during young adulthood using a set-shifting task and the elevated plus maze. Inhibitory parvalbumin-expressing (PV +) neuron counts were assessed in the mPFC and cerebellar lobules VI and VII (Purkinje cell layers), which are known to modulate cognition. VPA males had increased PV + counts in crus I and II of lobule VII. VPA males also had decreased parvalbumin-expressing neuron counts in the mPFC. It was also found that VPA-exposed rats, regardless of sex, had increased parvalbumin-expressing Purkinje cell counts in lobule VI. In males, this was associated with impaired intra-dimensional shifting on a set-shifting task. Purkinje cell over proliferation may be contributing to the previously observed increase in volume of Lobule VI. These findings suggest that altered inhibitory signaling in cerebellar-frontal circuits may contribute to the cognitive deficits that occur within ASD.

摘要

孕期接触丙戊酸(VPA,一种常见的抗癫痫药物)是自闭症谱系障碍(ASD)的一个风险因素。ASD患者的小脑常常出现变化,包括体积改变、神经回路改变以及浦肯野细胞数量变化。ASD的另一个特征是内侧前额叶皮质(mPFC)发生变化,该区域的兴奋/抑制平衡常常改变。本研究在孕期让大鼠接触高剂量的VPA,并在成年早期使用定势转换任务和高架十字迷宫评估其认知和焦虑样行为。对mPFC以及小脑小叶VI和VII(浦肯野细胞层)中表达小白蛋白的抑制性(PV +)神经元数量进行了评估,已知这些区域会调节认知。VPA雄性大鼠在小叶VII的 crus I和II中PV +数量增加。VPA雄性大鼠在mPFC中表达小白蛋白的神经元数量也减少。研究还发现,无论性别,接触VPA的大鼠在小叶VI中表达小白蛋白的浦肯野细胞数量增加。在雄性大鼠中,这与定势转换任务中的维度内转换受损有关。浦肯野细胞过度增殖可能是之前观察到的小叶VI体积增加的原因。这些发现表明,小脑 - 额叶回路中抑制性信号的改变可能导致了ASD患者出现的认知缺陷。

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