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Persistent luminescence nanoparticles functionalized by polymers bearing phosphonic acid anchors: synthesis, characterization, and in vivo behaviour

机译:持续发光纳米粒子功能化聚合物轴承膦酸锚:合成、表征和体内的行为

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Optical in vivo imaging has become a widely used technique and is still under development for clinical diagnostics and treatment applications. For further development of the field, researchers have put much effort into the development of inorganic nanoparticles (NPs) as imaging probes. In this trend, our laboratory developed ZnGa1.995O4Cr0.005 (ZGO) nanoparticles, which can emit a bright persistent luminescence signal through the tissue transparency window for dozens of minutes and can be activated in vivo with visible irradiation. These properties endow them with unique features, allowing us to recover information over a long-time study with in vivo imaging without any background. To target tissues of interest, ZGO must circulate long enough in the blood stream, a phenomenon which is limited by the mononuclear phagocyte system (MPS). Depending on their size, charge and coating, the NPs are sooner or later opsonized and stored into the main organs of the MPS (liver, spleen, and lungs). The NPs therefore have to be coated with a hydrophilic polymer to avoid this limitation. To this end, a new functionalization method using two different polyethylene glycol phosphonic acid polymers (a linear one, later named IpPEG and a branched one, later named pPEG) has been studied in this article. The coating has been optimized and characterized in various aqueous media. The behaviour of the newly functionalized NPs has been investigated in the presence of plasmatic proteins, and an in vivo biodistribution study has been performed. Among them ZGOpPEG exhibits a long circulation time, corresponding to low protein adsorption, while presenting an effective one-step process in aqueous medium with a low hydrodynamic diameter increase. This new method is much more advantageous than another strategy we reported previously that used a two-step PEG silane coating performed in an organic solvent (dimethylformamide) for which the final hydrodynamic diameter was twice the initial diameter.
机译:体内光学成像已成为广泛使用的技术和仍在发展临床诊断和治疗的应用。为该领域的进一步发展,研究人员将大部分精力投入发展吗无机纳米粒子(NPs)成像探针。在这一趋势,我们实验室开发ZnGa1.995O4Cr0.005 (ZGO)纳米粒子,可以发出明亮的持久发光信号通过组织数十个透明窗分钟,可以激活体内可见辐射。具有独特的特性,使我们恢复信息在体内的长期研究成像没有任何背景。感兴趣的,ZGO必须足够长的时间在流通血液,现象是有限的单核吞噬细胞系统(议员)。取决于他们的大小、电荷和涂层NPs是迟早调理和存储国会议员的主要器官(肝、脾和肺)。亲水聚合物来避免这种限制。为此,一个新的功能化方法使用两个不同的聚乙二醇膦酸聚合物(线性,后来IpPEG和命名分支,后来叫pPEG)进行了研究在这篇文章中。媒体和各水特征。新功能化NPs的行为在存在血浆的调查蛋白质,体内biodistribution研究已执行。循环时间长,相应的低蛋白质吸附,而提出一个有效的在水介质低的一步法水动力直径增加。比另一个更有利的策略我们以前报道,用一个两步挂钩硅烷涂层在有机溶剂中执行(二甲基甲酰胺)的决赛水动力直径是最初的两倍直径。

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