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Sandwich-Structured Upconversion Nanoprobes Coated with a Thin Silica Layer for Mitochondria-Targeted Cooperative Photodynamic Therapy for Solid Malignant Tumors

机译:夹层结构覆盖有薄二氧化硅层的薄二氧化硅层,用于线粒体靶向合作光动力治疗,用于固体恶性肿瘤

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摘要

Upconversion nanoparticles-based photodynamic nanotheranostic agents (UCNPs-PDT) have received great interest due to improved tissue penetration, weak autofluorescence, and low biotoxicity. However, conventional UCNPs-PDT are often limited by low energy transfer efficiency from UCNPs to photosensitizer (PS) molecules and insufficient generation and limited diffusion distance of reactive oxygen species (ROSs). Herein, an "all in one" nanotheranostic agent has been developed which has multicolor sandwich-structured UCNPs (SWUCNPs) as the core, a thin silica layer with a mitochondria-targeted group for loading dual PS as the medium layer, and polyethylene glycol-folic acid (PEG-FA) chains as the outer layer. Multicolor SWUCNPs simultaneously achieve two-photon fluorescence imaging and serve as energy donor for dual PS molecules. The thin luminescence layer and silica layer control most UCNPs activators and PS molecules in the effective energy transfer distance to guarantee a high energy transfer efficiency. Via FA-mediated endocytosis, the nanotheranostic agent is selectively endocytosed by cancer cells, is released from the endosome/lysosome, targets the mitochondria, and in situ produces ROSs under excitation from NIR, leading to significant mitochondria-mediated cell apoptosis. Furthermore, the established nanotheranostic agent shows tumor targetability, increased generation of ROSs, high PDT efficacy, significant cell apoptosis, minimal systemic cytotoxicity, and efficacious in vivo tumor inhibition.
机译:基于上转化的纳米颗粒基光动力纳米移植剂(UCNPS-PDT)由于改善的组织渗透,弱自发荧光和低生物毒性而受到巨大的兴趣。然而,常规的UCNPS-PDT通常受到来自UCNP的低能量转移效率的限制为光敏剂(PS)分子,并且活性氧物质(罗斯)的产生和有限扩散距离。在此,已经开发了“含有一个”纳米移植剂,其具有多色夹层结构的UCNP(Swucnps)作为芯,具有线粒体靶向基团的薄二氧化硅层,用于加载双PS作为介质层,以及聚乙二醇 - 叶酸(PEG-FA)链作为外层。多色Swucnps同时实现双光子荧光成像并用作双PS分子的能量供体。薄发光层和二氧化硅层控制大多数UCNP活化剂和PS分子在有效的能量转移距离中,以保证高能量转移效率。通过Fa介导的内吞作用,纳米抑制剂是通过癌细胞选择性地吞噬的,从内体/溶酶体释放,靶向线粒体,原位在NIR激发下产生罗斯,导致显着的线粒体介导的细胞凋亡。此外,已建立的纳米移植剂显示出肿瘤靶向性,增加罗斯的产生,高PDT疗效,显着细胞凋亡,最小的全身细胞毒性,以及体内肿瘤抑制的有效性。

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  • 来源
    《Analytical chemistry》 |2019年第13期|共9页
  • 作者单位

    Linyi Univ Collaborat Innovat Ctr Tumor Marker Detect Techno Shandong Prov Key Lab Detect Technol Tumor Marker Coll Chem &

    Chem Engn Linyi 276005 Shandong Peoples R China;

    Linyi Univ Collaborat Innovat Ctr Tumor Marker Detect Techno Shandong Prov Key Lab Detect Technol Tumor Marker Coll Chem &

    Chem Engn Linyi 276005 Shandong Peoples R China;

    Linyi Univ Collaborat Innovat Ctr Tumor Marker Detect Techno Shandong Prov Key Lab Detect Technol Tumor Marker Coll Chem &

    Chem Engn Linyi 276005 Shandong Peoples R China;

    Qingdao Univ Coll Chem &

    Chem Engn Shandong Sino Japanese Ctr Collaborat Res Carbon Qingdao 266071 Shandong Peoples R China;

    Linyi Univ Collaborat Innovat Ctr Tumor Marker Detect Techno Shandong Prov Key Lab Detect Technol Tumor Marker Coll Chem &

    Chem Engn Linyi 276005 Shandong 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;
  • 关键词

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