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人脐带间充质干细胞来源的神经元样细胞作为一种新的体外神经毒性筛选模型的研究:以磁铁矿纳米颗粒为例。

Neuron-Like Cells Generated from Human Umbilical Cord Lining-Derived Mesenchymal Stem Cells as a New In Vitro Model for Neuronal Toxicity Screening: Using Magnetite Nanoparticles as an Example.

机构信息

Laboratory of Clinical & Experimental Toxicology, Toxicology Unit, ICS Maugeri SpA-Benefit Corporation, IRCCS Pavia, Via Maugeri 10, 27100 Pavia, Italy.

Department of Obstetrics and Gynecology, Fondazione IRCCS Policlinico San Matteo and University of Pavia, 27100 Pavia, Italy.

出版信息

Int J Mol Sci. 2019 Dec 31;21(1):271. doi: 10.3390/ijms21010271.

Abstract

The wide employment of iron nanoparticles in environmental and occupational settings underlines their potential to enter the brain. Human cell-based systems are recommended as relevant models to reduce uncertainty and to improve prediction of human toxicity. This study aimed at demonstrating the in vitro differentiation of the human umbilical cord lining-derived-mesenchymal stem cells (hCL-MSCs) into neuron-like cells (hNLCs) and the benefit of using them as an ideal primary cell source of human origin for the neuronal toxicity of FeONPs (magnetite-nanoparticles). Neuron-like phenotype was confirmed by: live morphology; Nissl body staining; protein expression of different neuronal-specific markers (immunofluorescent staining), at different maturation stages (i.e., day-3-early and day-8-full differentiated), namely β-tubulin III, MAP-2, enolase (NSE), glial protein, and almost no nestin and SOX-2 expression. Synaptic makers (SYN, GAP43, and PSD95) were also expressed. FeONPs determined a concentration- and time-dependent reduction of hNLCs viability (by ATP and the Trypan Blue test). Cell density decreased (20-50%) and apoptotic effects were detected at ≥10 μg/mL in both types of differentiated hNLCs. Three-day-differentiated hNLCs were more susceptible (toxicity appeared early and lasted for up to 48 h) than 8-day-differentiated cells (delayed effects). The study demonstrated that (i) hCL-MSCs easily differentiated into neuronal-like cells; (ii) the hNCLs susceptibility to FeONPs; and (iii) human primary cultures of neurons are new in vitro model for NP evaluation.

摘要

铁纳米粒子在环境和职业环境中的广泛应用突出了它们进入大脑的潜力。推荐使用基于人类细胞的系统作为相关模型,以减少不确定性并提高对人类毒性的预测。本研究旨在证明人脐带衬里衍生间充质干细胞(hCL-MSCs)向神经元样细胞(hNLCs)的体外分化,以及将其用作人类来源神经元毒性铁纳米粒子(磁铁矿纳米粒子)的理想原代细胞来源的益处。通过以下方式确认神经元样表型:活细胞形态;尼氏体染色;不同神经元特异性标志物(免疫荧光染色)的蛋白表达,在不同成熟阶段(即第 3 天-早期和第 8 天-完全分化),即β-微管蛋白 III、MAP-2、烯醇酶(NSE)、神经胶质蛋白,以及几乎没有巢蛋白和 SOX-2 的表达。突触标志物(SYN、GAP43 和 PSD95)也被表达。FeONPs 确定了 hNLCs 活力的浓度和时间依赖性降低(通过 ATP 和台盼蓝试验)。在两种分化的 hNLCs 中,细胞密度均降低(20-50%),并且在≥10μg/mL 时检测到凋亡作用。3 天分化的 hNLCs比 8 天分化的细胞(延迟作用)更容易受到影响(毒性出现较早,持续时间长达 48 小时)。该研究表明:(i)hCL-MSCs 易于分化为神经元样细胞;(ii)hNLCs 对 FeONPs 的敏感性;(iii)人类原代神经元培养物是 NP 评价的新型体外模型。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3c3c/6982086/488a9e963f61/ijms-21-00271-g001.jpg

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