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Splenic Capture and In Vivo Intracellular Biodegradation of Biological-Grade Graphene Oxide Sheets

机译:脾捕获和体内生物级石墨烯氧化物片的细胞内生物降解

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摘要

Carbon nanomaterials, including 2D graphene-based materials, have shown promising applicability to drug delivery, tissue engineering, diagnostics, and various other biomedical areas. However, to exploit the benefits of these materials in some of the areas mentioned, it is necessary to understand their possible toxicological implications and long-term fate in vivo . We previously demonstrated that following intravenous administration, 2D graphene oxide (GO) nanosheets were largely excreted via the kidneys; however, a small but significant portion of the material was sequestered in the spleen. Herein, we interrogate the potential consequences of this accumulation and the fate of the spleen-residing GO over a period of nine months. We show that our thoroughly characterized GO materials are not associated with any detectable pathological consequences in the spleen. Using confocal Raman mapping of tissue sections, we determine the sub-organ biodistribution of GO at various time points after administration. The cells largely responsible for taking up the material are confirmed using immunohistochemistry coupled with Raman spectroscopy, and transmission electron microscopy (TEM). This combination of techniques identified cells of the splenic marginal zone as the main site of GO bioaccumulation. In addition, through analyses using both bright-field TEM coupled with electron diffraction and Raman spectroscopy, we reveal direct evidence of in vivo intracellular biodegradation of GO sheets with ultrastructural precision. This work offers critical information about biological processing and degradation of thin GO sheets by normal mammalian tissue, indicating that further development and exploitation of GO in biomedicine would be possible.
机译:碳纳米材料(包括2D石墨烯基材料)已经显示出对药物递送,组织工程,诊断和各种其他生物医学领域的有希望的适用性。然而,为了利用这些材料在提到的一些地区的利益,有必要了解他们在体内可能的毒理学影响和长期命运。我们以前证明,静脉内给药后,2D石墨烯(GO)纳米片在很大程度上通过肾脏排出;然而,在脾脏中螯合了一小部分的材料。在此,我们询问了这种积累的潜在后果,脾居住的命运在九个月内进行了九个月。我们表明,我们完全表征的GO材料与脾脏中任何可检测的病理后果无关。使用组织切片的共聚焦拉曼映射,我们确定在给药后各个时间点的转移的子器官生物分布。使用免疫组织化学与拉曼光谱和透射电子显微镜(TEM)耦合的免疫组化来确认大部分负责占据材料的细胞。这种技术的组合确定了脾脏边缘区的细胞作为Go生物累积的主要部位。另外,通过使用亮场TEM与电子衍射和拉曼光谱相结合的分析,我们揭示了具有超微结构精度的Vivo细胞内生物降解的直接证据。这项工作提供了正常哺乳动物组织的有关薄Go床单的生物处理和降解的关键信息,表明可以进一步发展和剥削生物医学的进一步发展和开发。

著录项

  • 来源
    《ACS nano》 |2020年第8期|共19页
  • 作者单位

    Nanomedicine Lab National Graphene Institute and Faculty of Biology Medicine &

    Health The University of Manchester;

    Nanomedicine Lab National Graphene Institute and Faculty of Biology Medicine &

    Health The University of Manchester;

    Department of Materials School of Natural Sciences The University of Manchester;

    Nanomedicine Lab National Graphene Institute and Faculty of Biology Medicine &

    Health The University of Manchester;

    Nanomedicine Lab National Graphene Institute and Faculty of Biology Medicine &

    Health The University of Manchester;

    Nanomedicine Lab National Graphene Institute and Faculty of Biology Medicine &

    Health The University of Manchester;

    Lydia Becker Institute of Immunology and Inflammation and Division of Infection Immunity and Respiratory Medicine School of Biological Sciences Faculty of Biology Medicine and Health The University of Manchester;

    Lydia Becker Institute of Immunology and Inflammation and Division of Infection Immunity and Respiratory Medicine School of Biological Sciences Faculty of Biology Medicine and Health The University of Manchester;

    Department of Materials School of Natural Sciences The University of Manchester;

    Nanomedicine Lab National Graphene Institute and Faculty of Biology Medicine &

    Health The University of Manchester;

    Nanomedicine Lab National Graphene Institute and Faculty of Biology Medicine &

    Health The University of Manchester;

  • 收录信息
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 分子物理学、原子物理学;
  • 关键词

    2D materials; degradation; macrophage; toxicology; nanomedicine;

    机译:2D材料;降解;巨噬细胞;毒理学;纳米医生;

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