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产后氟西汀治疗改变海马区周围神经网的形成和维持。

Postnatal Fluoxetine Treatment Alters Perineuronal Net Formation and Maintenance in the Hippocampus.

机构信息

Department of Biological Sciences, Tata Institute of Fundamental Research, Mumbai 400005, India.

Department of Biological Sciences, Tata Institute of Fundamental Research, Mumbai 400005, India

出版信息

eNeuro. 2021 Apr 13;8(2). doi: 10.1523/ENEURO.0424-20.2021. Print 2021 Mar-Apr.

Abstract

Elevation of serotonin via postnatal fluoxetine (PNFlx) treatment during critical temporal windows is hypothesized to perturb the development of limbic circuits thus establishing a substratum for persistent disruption of mood-related behavior. We examined the impact of PNFlx treatment on the formation and maintenance of perineuronal nets (PNNs), extracellular matrix (ECM) structures that deposit primarily around inhibitory interneurons, and mark the closure of critical period plasticity. PNFlx treatment evoked a significant decline in PNN number, with a robust reduction in PNNs deposited around parvalbumin (PV) interneurons, within the CA1 and CA3 hippocampal subfields at postnatal day (P)21 in Sprague Dawley rat pups. While the reduction in CA1 subfield PNN number was still observed in adulthood, we observed no change in colocalization of PV-positive interneurons with PNNs in the hippocampi of adult PNFlx animals. PNFlx treatment did not alter hippocampal PV, calretinin (CalR), or Reelin-positive neuron numbers in PNFlx animals at P21 or in adulthood. We did observe a small, but significant increase in somatostatin (SST)-positive interneurons in the DG subfield of PNFlx-treated animals in adulthood. This was accompanied by altered GABA-A receptor subunit composition, increased dendritic complexity of apical dendrites of CA1 pyramidal neurons, and enhanced neuronal activation revealed by increased c-Fos-positive cell numbers within hippocampi of PNFlx-treated animals in adulthood. These results indicate that PNFlx treatment alters the formation of PNNs within the hippocampus, raising the possibility of a disruption of excitation-inhibition (E/I) balance within this key limbic brain region.

摘要

通过产后氟西汀(PNFlx)治疗在关键时间窗口升高 5-羟色胺,被假设为扰乱边缘回路的发育,从而为情绪相关行为的持续破坏建立基础。我们研究了 PNFlx 治疗对周围神经网(PNNs)形成和维持的影响,PNNs 是主要沉积在抑制性中间神经元周围的细胞外基质(ECM)结构,标志着关键期可塑性的关闭。PNFlx 治疗引起 PNN 数量显著下降,在 Sprague Dawley 幼鼠的 CA1 和 CA3 海马亚区,PNFlx 处理后第 21 天,PV 中间神经元周围的 PNN 数量明显减少。虽然 CA1 亚区 PNN 数量的减少在成年期仍然存在,但我们没有观察到成年 PNFlx 动物海马中 PV 阳性中间神经元与 PNN 的共定位发生变化。PNFlx 处理没有改变 P21 或成年期 PNFlx 动物海马中的 PV、钙结合蛋白(CalR)或 Reelin 阳性神经元数量。我们确实观察到成年 PNFlx 处理动物的 DG 亚区中,SST 阳性中间神经元数量略有增加,但具有统计学意义。这伴随着 GABA-A 受体亚基组成的改变、CA1 锥体神经元顶树突的分支复杂性增加,以及成年期 PNFlx 处理动物海马中 c-Fos 阳性细胞数量增加所揭示的神经元激活增强。这些结果表明,PNFlx 处理改变了海马内 PNNs 的形成,增加了兴奋-抑制(E/I)平衡在这个关键的边缘脑区被破坏的可能性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/bfaf/8046023/611279cc732e/SN-ENUJ210055F002.jpg

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