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Vascular endothelial cells and pulmonary epithelial cells: Uptake and response to metal oxide nanoparticles.

机译:血管内皮细胞和肺上皮细胞:对金属氧化物纳米颗粒的吸收和反应。

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摘要

Nanomaterials are promoted as a promising technology in highly diverse applications, but concerns about risks of these materials have stimulated extensive research on the adverse effects of manufactured nanoparticles. Our research utilized ex vivo tissues to study quantification of unlabeled nanoparticles in biological media and in vitro cultures of human cells, treated with suspensions of low-solubility metal oxide materials, to study uptake, cell signaling, and gene regulation. The effects of nanoparticles on the cardiovascular system occur because inhaled nanoparticles may enter systemic circulation, or are directly injected into systemic circulation for medical applications, causing adverse health effects. Silicon dioxide (SiO2) particles with sizes between 20-100 nm were used in our studies because they have many commercial and medical applications and can be readily modified with surface functional groups. Our hypothesis is two-fold. First, we hypothesize that tissue uptake and deposition of SiO 2 nanoparticles can be measured by sedimentation field-flow fractionation (SdFFF) after particle isolation using enzyme digestion. We also hypothesize that the adverse effects associated with nanoparticle exposures are greater in vascular cells than pulmonary and colorectal cell lines, due to the formation of reactive oxygen species, which may stimulate apoptosis. The results presented here demonstrate the cellular uptake of nano and submicron-sized SiO 2 using the traditional methods of microscopy. Additionally, the method of SdFFF, which is typically used to separate macromolecules, colloids, and particles, was used in combination with enzyme digestion to provide a novel, useful method to simultaneously measure both the size and concentration of particles in tissues. The toxic effects of metal oxide particle treatment on vascular, pulmonary and colon cells were evaluated. Significant cytotoxicity and inflammation were observed with vascular endothelial cells, but little to no adverse effects were seen in pulmonary and colon cancer epithelial cells at concentrations of 1-316 mug/cm2. Nano-sized SiO2 caused apoptosis in vascular endothelial cells that was ameliorated by pretreatment with 5 mM of the antioxidant, N-acetyl-L-cysteine. Our results show that exposures of endothelial cells to high concentrations of nano-sized SiO2 may have serious adverse cardiovascular consequences. Furthermore, these results provide insights into treatments, such as the use of antioxidants, for persons exposed to significant levels of metal oxide nanoparticles.
机译:纳米材料在高度多样化的应用中被推广为一种有前途的技术,但是对这些材料的风险的担忧刺激了人们对人造纳米颗粒的不利影响进行广泛的研究。我们的研究利用离体组织研究生物介质和人细胞体外培养物中未标记的纳米颗粒的定量,并用低溶解度金属氧化物材料的悬浮液处理,以研究摄取,细胞信号转导和基因调控。纳米颗粒对心血管系统的影响之所以发生,是因为吸入的纳米颗粒可能进入体循环,或直接注入体循环以用于医疗应用,从而对健康产生不利影响。在我们的研究中使用尺寸在20至100 nm之间的二氧化硅(SiO2)颗粒,因为它们具有许多商业和医学应用,并且可以很容易地被表面官能团改性。我们的假设是双重的。首先,我们假设可以通过使用酶消化分离颗粒后的沉降场流分级分离(SdFFF)来测量SiO 2纳米颗粒的组织摄取和沉积。我们还假设与纳米颗粒暴露相关的不良反应在血管细胞中比肺和结肠直肠细胞系要大,这是由于活性氧的形成可能会刺激细胞凋亡。此处显示的结果证明了使用传统显微镜方法对纳米和亚微米级SiO 2的细胞吸收。此外,通常用于分离大分子,胶体和颗粒的SdFFF方法与酶消化结合使用,可提供一种新颖,有用的方法,可同时测量组织中颗粒的大小和浓度。评价了金属氧化物颗粒处理对血管,肺和结肠细胞的毒性作用。在血管内皮细胞中观察到了明显的细胞毒性和炎症,但是在浓度为1-316马克杯/平方厘米的肺和结肠癌上皮细胞中几乎没有观察到不良反应。纳米SiO2引起血管内皮细胞凋亡,通过用5 mM的抗氧化剂N-乙酰基-L-半胱氨酸进行预处理可以缓解这种情况。我们的结果表明,内皮细胞暴露于高浓度的纳米级SiO2可能会对心血管系统造成严重不利影响。此外,这些结果为接触大量金属氧化物纳米粒子的人提供了治疗方法的见解,例如使用抗氧化剂。

著录项

  • 作者单位

    The University of Utah.;

  • 授予单位 The University of Utah.;
  • 学科 Toxicology.;Environmental science.
  • 学位 Ph.D.
  • 年度 2009
  • 页码 102 p.
  • 总页数 102
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

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