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产前应激以性别特异性方式改变小鼠后代的背侧纹状体发育和胎盘功能。

Prenatal stress alters mouse offspring dorsal striatal development and placental function in sex-specific ways.

作者信息

Maurer Sara V, Hing Benjamin W Q, Lussier Stephanie, Radhakrishna Sreya, Davis Jada L B, Abbott Parker W, Michaelson Jacob J, Stevens Hanna E

机构信息

Department of Psychiatry, University of Iowa Carver College of Medicine, Iowa City, IA, 52246, USA; Iowa Neuroscience Institute, University of Iowa, Iowa City, IA, 52246, USA.

Department of Psychiatry, University of Iowa Carver College of Medicine, Iowa City, IA, 52246, USA; Yale Child Study Center, Yale School of Medicine, New Haven, CT, 06510, USA; SL is now with Moderna, USA.

出版信息

J Psychiatr Res. 2025 Feb;182:149-160. doi: 10.1016/j.jpsychires.2024.12.048. Epub 2025 Jan 1.

Abstract

Prenatal stress is a risk factor for neurodevelopmental disorders (NDDs), including autism spectrum disorder (ASD). However, how early stress modification of brain development contributes to this pathophysiology is poorly understood. Ventral forebrain regions such as dorsal striatum are of particular interest: dorsal striatum modulates movement and cognition, is altered in NDDs, and has a primarily GABAergic population. Here, we examine effects of prenatal stress on adult movement, cognition, and dorsal striatum neurobiology in mice using striatal-dependent behavioral assays, immunohistochemistry, embryonic ventral forebrain transcriptomics, and placental transcriptomics. We found prenatal stress affected adult procedural, habit, and reversal learning in sex-specific ways. Stress also increased adult dorsal striatal GABAergic neurons - an effect largely driven by males. We sought to examine the developmental origins of these adult brain changes. We found similar sex-specific dorsal striatal cellular changes in earlier points of development. The dorsal striatum primordium--embryonic ventral forebrain-showed that prenatal stress increased DNA replication and cell cycle pathways in male but not female transcriptomics and cellular biology. Unique signatures may have arisen from male-female placental differences. Stress-induced placental transcriptomics showed upregulated morphogenesis pathways in males while females downregulated morphogenic, hormonal, and cellular response pathways. Our findings suggest that prenatal stress could affect placenta function and also alter the GABAergic population of dorsal striatum differentially between the sexes.

摘要

产前应激是神经发育障碍(NDDs)的一个风险因素,包括自闭症谱系障碍(ASD)。然而,早期应激如何影响大脑发育并导致这种病理生理学变化,目前还知之甚少。腹侧前脑区域如背侧纹状体尤其值得关注:背侧纹状体调节运动和认知,在神经发育障碍中会发生改变,且主要由γ-氨基丁酸(GABA)能神经元组成。在这里,我们使用依赖纹状体的行为测定、免疫组织化学、胚胎腹侧前脑转录组学和胎盘转录组学,研究产前应激对成年小鼠运动、认知和背侧纹状体神经生物学的影响。我们发现产前应激以性别特异性方式影响成年小鼠的程序性学习、习惯学习和逆向学习。应激还增加了成年小鼠背侧纹状体的GABA能神经元——这一效应在很大程度上由雄性驱动。我们试图探究这些成年大脑变化的发育起源。我们发现在发育的早期阶段,背侧纹状体也存在类似的性别特异性细胞变化。背侧纹状体原基——胚胎腹侧前脑——显示产前应激在雄性而非雌性的转录组学和细胞生物学中增加了DNA复制和细胞周期途径。独特的特征可能源于雄性和雌性胎盘的差异。应激诱导的胎盘转录组学显示,雄性的形态发生途径上调,而雌性的形态发生、激素和细胞反应途径下调。我们的研究结果表明,产前应激可能会影响胎盘功能,并且还会在性别之间差异性地改变背侧纹状体的GABA能神经元群体。

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