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纳米银对幼鼠大脑中谷氨酸能 NMDA 受体复合物的早期和延迟影响。

Early and Delayed Impact of Nanosilver on the Glutamatergic NMDA Receptor Complex in Immature Rat Brain.

机构信息

Laboratory of Pathoneurochemistry, Department of Neurochemistr, Mossakowski Medical Research Institute, Polish Academy of Sciences, Pawińskiego 5, 02-106 Warsaw, Poland.

Electron Microscopy Platform, Mossakowski Medical Research Institute, Polish Academy of Sciences, Pawińskiego 5, 02-106 Warsaw, Poland.

出版信息

Int J Mol Sci. 2021 Mar 17;22(6):3067. doi: 10.3390/ijms22063067.

Abstract

Silver nanoparticles (AgNPs) are the one of the most extensively used nanomaterials. The strong antimicrobial properties of AgNPs have led to their use in a wide range of medical and consumer products. Although the neurotoxicity of AgNPs has been confirmed, the molecular mechanisms have not been extensively studied, particularly in immature organisms. Based on information gained from previous in vitro studies, in the present work, we examine whether ionotropic NMDA glutamate receptors contribute to AgNP-induced neurotoxicity in an animal model of exposure. In brains of immature rats subjected to a low dose of AgNPs, we identified ultrastructural and molecular alterations in the postsynaptic region of synapses where NMDA receptors are localized as a multiprotein complex. We revealed decreased expression of several NMDA receptor complex-related proteins, such as GluN1 and GluN2B subunits, scaffolding proteins PSD95 and SynGAP, as well as neuronal nitric oxide synthase (nNOS). Elucidating the changes in NMDA receptor-mediated molecular mechanisms induced by AgNPs, we also identified downregulation of the GluN2B-PSD95-nNOS-cGMP signaling pathway which maintains LTP/LTD processes underlying learning and memory formation during development. This observation is accompanied by decreased density of NMDA receptors, as assessed by a radioligand binding assay. The observed effects are reversible over the post-exposure time. This investigation reveals that NMDA receptors in immature rats are a target of AgNPs, thereby indicating the potential health hazard for children and infants resulting from the extensive use of products containing AgNPs.

摘要

纳米银颗粒(AgNPs)是应用最广泛的纳米材料之一。AgNPs 具有很强的抗菌性能,因此被广泛应用于医疗和消费品领域。虽然 AgNPs 的神经毒性已得到证实,但分子机制尚未得到广泛研究,尤其是在未成熟的生物体中。基于之前体外研究获得的信息,本研究在暴露于 AgNPs 的动物模型中,检查离子型 NMDA 谷氨酸受体是否参与 AgNP 诱导的神经毒性。在接受低剂量 AgNPs 处理的未成熟大鼠的大脑中,我们在 NMDA 受体定位于突触后区的突触中发现了超微结构和分子改变,NMDA 受体作为一个多蛋白复合物存在。我们发现几种 NMDA 受体复合物相关蛋白的表达减少,如 GluN1 和 GluN2B 亚基、支架蛋白 PSD95 和 SynGAP 以及神经元型一氧化氮合酶(nNOS)。阐明 AgNPs 诱导的 NMDA 受体介导的分子机制变化,我们还发现下调了 GluN2B-PSD95-nNOS-cGMP 信号通路,该信号通路在发育过程中维持着学习和记忆形成的 LTP/LTD 过程。这种观察结果伴随着 NMDA 受体密度的降低,通过放射性配体结合测定进行评估。在暴露后的时间内,观察到的效应是可逆的。这项研究表明,未成熟大鼠的 NMDA 受体是 AgNPs 的靶标,从而表明由于广泛使用含有 AgNPs 的产品,儿童和婴儿可能面临潜在的健康危害。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/780d/8002467/06b1b48abba6/ijms-22-03067-g001.jpg

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