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首页> 外文期刊>Analytical chemistry >Design of a New Near-Infrared Ratiometric Fluorescent Nanoprobe for Real-Time Imaging of Superoxide Anions and Hydroxyl Radicals in Live Cells and in Situ Tracing of the Inflammation Process in Vivo
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Design of a New Near-Infrared Ratiometric Fluorescent Nanoprobe for Real-Time Imaging of Superoxide Anions and Hydroxyl Radicals in Live Cells and in Situ Tracing of the Inflammation Process in Vivo

机译:设计新的近红外比率荧光纳米孔,用于实时细胞中超氧化物阴离子和羟基自由基的实时成像,以及体内炎症过程的原位追踪

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摘要

The superoxide anion (O-2(center dot-)) and hydroxyl radical ((OH)-O-center dot) are important reactive oxygen species (ROS) used as biomarkers in physiological and pathological processes. ROS generation is closely related to the development of a variety of inflammatory diseases. However, the changes of ROS are difficult to ascertain with in situ tracing of the inflammation process by real-time monitoring, owing to the short half-lives of ROS and high tissue autofluorescence in vivo. Here we developed a new near-infrared (NIR) ratiometric fluorescence imaging approach by using a Forster resonance energy transfer (FRET)-based ratiometric fluorescent nanoprobe for real-time monitoring of O-2(center dot-) and (OH)-O-center dot generation and also by using in situ tracing of the inflammation process in vivo. The proposed nanoprobe was composed of PEG functionalized GQDs as the energy donor connecting to hydroIR783, serving as both the O-2(center dot-)/(OH)-O-center dot recognizing ligand and the energy acceptor. The nanoprobe not only exhibited a fast response to O-2(center dot-) and (OH)-O-center dot but also presented good biocomapatibility as well as a high photostability and signal-to-noise ratio. We have demonstrated that the proposed NIR ratiometric fluorescent nanoprobe can monitor the changes of O-2(center dot-) and (OH)-O-center dot in living RAW 264.7 cells via a drug mediating inflammation model and further realized visual monitoring of the change of O-2(center dot-) and (OH)-O-center dot in mice for in situ tracing of the inflammation process. Our design may provide a new paradigm for long-term and real-time imaging applications for in vivo tracing of the pathological process related to the inflammatory diseases.
机译:超氧化物阴离子(O-2(中心点))和羟基自由基((OH)-O-中心点)是在生理和病理过程中用作生物标志物的重要反应性氧物质(ROS)。 ROS生成与各种炎症性疾病的发展密切相关。然而,由于VIVO中的ROS和高组织自发荧光短暂的半衰期,难以确定ROS的变化难以确定炎症过程的原位追踪。在这里,我们通过使用Forster Arsonance能量转移(FRET)的比例荧光纳米孔开发了一种新的近红外(NIR)比率荧光成像方法,用于实时监测O-2(中心DOT-)和(OH)-O - Center Dot发电,也通过使用体内炎症过程的原位追踪。所提出的纳米孔由PEG官能化GQD组成,作为连接到HydroiR783的能量供体组成,用作O-2(中心点 - )/(OH)-O中心点识别配体和能量受体。 Nanopobe不仅表现出对O-2(中心点)和(OH)-O中心点的快速响应,而且还呈现出良好的生物涂覆性以及高光稳定性和信噪比。我们已经证明,所提出的鼻腔比例荧光纳米孔可以通过介质介导的炎症模型监测Live Raw 264.7细胞中的O-2(中心点)和(OH)-O-中心点的变化,进一步实现了视觉监测炎症过程原位描绘的小鼠中O-2(中心点)和(OH)-O中心点的变化。我们的设计可以为长期和实时成像应用提供新的范例,用于体内追踪与炎症性疾病有关的病理过程。

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  • 来源
    《Analytical chemistry》 |2018年第7期|共9页
  • 作者单位

    Guangxi Normal Univ Coll Chem &

    Pharm State Key Lab Chem &

    Mol Engn Med Resources Guilin 541004 Peoples R China;

    Guangxi Normal Univ Coll Chem &

    Pharm State Key Lab Chem &

    Mol Engn Med Resources Guilin 541004 Peoples R China;

    Guangxi Normal Univ Coll Chem &

    Pharm State Key Lab Chem &

    Mol Engn Med Resources Guilin 541004 Peoples R China;

    Guangxi Normal Univ Coll Chem &

    Pharm State Key Lab Chem &

    Mol Engn Med Resources Guilin 541004 Peoples R China;

    Guangxi Normal Univ Coll Chem &

    Pharm State Key Lab Chem &

    Mol Engn Med Resources Guilin 541004 Peoples R China;

    Guangxi Normal Univ Coll Chem &

    Pharm State Key Lab Chem &

    Mol Engn Med Resources Guilin 541004 Peoples R China;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 分析化学;
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