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石墨烯类纳米材料在心肌细胞中的细胞毒性和内化作用的差异。

Differential cytotoxicity and internalization of graphene family nanomaterials in myocardial cells.

机构信息

Laboratorio de Nanotecnología Ambiental, Centro del Agua para América Latina y el Caribe, Tecnológico de Monterrey, Monterrey, 64849, Mexico.

Department of Chemistry, Universityof Oxford, South Parks Road, Oxford OX1 3QZ, UK.

出版信息

Mater Sci Eng C Mater Biol Appl. 2017 Apr 1;73:633-642. doi: 10.1016/j.msec.2016.12.080. Epub 2016 Dec 23.

Abstract

Given the well-known physical properties of graphene oxide (GO), numerous applications for this novel nanomaterial have been recently envisioned to improve the performance of biomedical devices. However, the toxicological assessment of GO, which strongly depends on the used material and the studied cell line, is a fundamental task that needs to be performed prior to its use in biomedical applications. Therefore, the toxicological characterization of GO is still ongoing. This study contributes to this, aiming to synthesize and characterize GO particles and thus investigate their toxic effects in myocardial cells. Herein, GO particles were produced from graphite using the Tour method and subsequent mild reduction was carried out to obtain low-reduced GO (LRGO) particles. A qualitative analysis of the viability, cellular uptake, and internalization of particles was carried out using GO (54% content of oxygen) and LRGO (37% content of oxygen) and graphite. GO and LRGO reduce the viability of cardiac cells at IC of 652.1±1.2 and 129.4±1.2μg/mL, respectively. This shows that LRGO particles produce a five-fold increase in cytotoxicity when compared to GO. The cell uptake pattern of GO and LRGO particles demonstrated that cardiac cells retain a similar complexity to control cells. Morphological alterations examined with electron microscopy showed that internalization by GO and LRGO-treated cells (100μg/mL) occurred affecting the cell structure. These results suggest that the viability of H9c2 cells can be associated with the surface chemistry of GO and LRGO, as defined by the amount of oxygen functionalities, the number of graphitic domains, and the size of particles. High angle annular dark-field scanning transmission electron microscopy, dynamic light-scattering, Fourier-transform infrared, Raman, and X-ray photoelectron spectroscopies were used to characterize the as-prepared materials.

摘要

鉴于氧化石墨烯(GO)众所周知的物理性质,最近人们设想了许多应用这种新型纳米材料的方法,以提高生物医学设备的性能。然而,GO 的毒理学评估强烈依赖于所使用的材料和所研究的细胞系,这是在其用于生物医学应用之前必须进行的基本任务。因此,GO 的毒理学特征仍在进行中。本研究旨在合成和表征 GO 颗粒,并研究其在心肌细胞中的毒性作用,为此做出了贡献。在此,使用 Tour 法从石墨生产 GO 颗粒,然后进行温和还原以获得低还原 GO(LRGO)颗粒。使用 GO(54%的氧含量)和 LRGO(37%的氧含量)和石墨对颗粒的细胞活力、摄取和内化进行了定性分析。GO 和 LRGO 将心肌细胞的活力分别降低到 IC 50 值为 652.1±1.2μg/mL 和 129.4±1.2μg/mL。这表明 LRGO 颗粒的细胞毒性比 GO 增加了五倍。GO 和 LRGO 颗粒的细胞摄取模式表明,心肌细胞保持与对照细胞相似的复杂性。电子显微镜检查的形态变化表明,GO 和 LRGO 处理的细胞(100μg/mL)的内化会影响细胞结构。这些结果表明,H9c2 细胞的活力可以与 GO 和 LRGO 的表面化学性质相关联,这由氧官能团的数量、石墨化域的数量和颗粒的大小来定义。高角度环形暗场扫描透射电子显微镜、动态光散射、傅里叶变换红外、拉曼和 X 射线光电子能谱用于表征所制备的材料。

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