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Microarray assisted toxicological investigations of boron carbide nanoparticles on human primary alveolar epithelial cells

机译:微阵列辅助硼碳化硼纳米粒子对人原发性肺泡上皮细胞的毒理学研究

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It is important to understand the adverse effects of nanoparticles on human health and to prepare risk reports for widely used nanoscale materials. Synthesis, characterization and cytotoxicity evaluation of B4C nanoparticles were performed on HPAEpiC since, first encounter with nanoparticles would generally happen through lung by inhaling chemicals. B4C nanoparticles were synthesized via chemical vapor deposition techniques and characterized by using transmission electron microscope (TEM), scanning electron microscope (SEM) and X-ray crystallography (XRD). 3-(4,5-dimethyl-thiazol-2-yl) 2,5-diphenyltetrazolium bromide (MTT), lactate dehydrogenase (LDH) and neutral red (NR) tests were used to analyze cell viability and cytotoxicity against nanoparticles exposure. Microarray analysis was used to discover whole genome effects of B4C NPs on gene expressions changes of HPAEpiC cells. Then, the database for annotation, visualization and integrated discovery (DAVID) analysis was performed to understand relationships between gene pathways and nanoparticle exposure. Finally, cytotoxicity analysis revealed that IC20 value for boron carbide (B4C) nanoparticles was 202.525 mg/L. According to microarray analysis 32 genes expression change significantly (FC = 2) over 40,000 genes scanning. The gene pathways analysis showed that boron carbide (B4C) nanoparticles mostly affect amino acid biosynthesis process, TGF-beta signaling pathway and developmental proteins regulation. In conclusion, our results supported for the first time that boron carbide (B4C) nanoparticles could be used as a safe nanomaterial in both pharmacological and medical applications.
机译:重要的是要了解纳米颗粒对人体健康的不利影响,并为广泛使用的纳米级材料制备风险报告。 B4C纳米颗粒对HPAPIC进行的合成,表征和细胞毒性评价,因为,通过吸入化学品通常通过肺部进行腹腔进行的首次遇到。通过化学气相沉积技术合成B4C纳米颗粒,其特征在于使用透射电子显微镜(TEM),扫描电子显微镜(SEM)和X射线晶体学(XRD)。 3-(4,5-二甲基 - 噻唑-2-基)2,5-二苯基四唑溴(MTT),使用乳酸脱氢酶(LDH)和中性红色(NR)试验来分析细胞活力和细胞毒性,对纳米颗粒暴露。微阵列分析用于发现B4C NP对HPAepic细胞的基因表达变化的全基因组效应。然后,进行注释,可视化和集成发现(DAVID)分析的数据库以了解基因途径和纳米粒子暴露之间的关系。最后,细胞毒性分析显示碳化硼(B4C)纳米颗粒的IC20值为202.525mg / L.根据微阵列分析32基因表达显着变化(Fc& = 2)超过40,000个基因扫描。基因途径分析表明,碳化硼(B4C)纳米颗粒主要影响氨基酸生物合成过程,TGF-Beta信号传导途径和发育蛋白调节。总之,我们的结果首次支持碳化硼(B4C)纳米颗粒可以用作药理学和医疗应用中的安全纳米材料。

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