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Bone-targeting carbon dots: effect of nitrogen-doping on binding affinity

机译:骨靶向碳点:氮掺杂对结合亲和力的影响

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摘要

Novel fluorescent carbon dots (CDs) for bone imaging were fabricated via a facile hydrothermal method using alendronate in the absence of a nitrogen-doping precursor to enhance bone affinity. One-step synthesized alendronate-based CDs (Alen-CDs) had strong binding activity for calcium-deficient hydroxyapatite (CDHA, the mineral component of bones) scaffold, rat femur, and bone structures of live zebrafish. This was attributed to the bisphosphonate group present on the CD surface, even after carbonization. For comparison, the surface effects of nitrogen-doped CDs obtained using ethylenediamine (EDA), i.e., Alen-EDA-CDs, were also investigated, focusing on the targeting ability of distinct surface functional groups when compared with Alen-CDs. An in vivo study to assess the impact on bone affinity revealed that Alen-CDs effectively accumulated in the bone structures of live zebrafish larvae after microinjections, as well as in the bone tissues of femur extracted from rats. Moreover, Alen-CD-treated zebrafish larvae had superior toleration, retaining skeletal fluorescence for 7 days post-injection (dpi). The sustainable capability, surpassing that of Alizarin Red S, suggests that Alen-CDs have the potential for targeted drug delivery to damaged bone tissues and provides motivation for additional in vivo investigations. To our knowledge, this is the first in vitro, ex vivo, and in vivo demonstration of direct bone-targeted deliveries, supporting the use of fluorescent CDs in the treatment of various bone diseases such as osteoporosis, Paget's disease, and metastatic bone cancer.
机译:通过在不存在氮气掺杂前体的情况下,通过体内ronate制造用于骨成像的新型荧光碳点(CDS),以增强骨亲和力。一步合成的基于Alendronate的CDS(ALEN-CDS)对钙缺乏的羟基磷灰石(CDHA,骨骼成分)支架,大鼠股骨和活斑马鱼骨结构具有较强的结合活性。这归因于在Cd表面上存在的双膦酸盐基团,即使在碳化之后也是如此。为了比较,还研究了使用乙二胺(EDA),即Alen-EDA-CDS获得的氮掺杂Cd的表面效应,与Alen-Cds相比,聚焦在不同表面官能团的靶向能力。一个体内研究,评估对骨亲和力的影响表明,在微量注射症后,ALEN-CD在活斑马鱼幼虫的骨骼结构中积累,以及从大鼠提取的股骨的骨组织中。此外,Alen-CD处理的斑马鱼幼虫具有优异的耐受性,保留骨骼荧光7天注射后7天(DPI)。可持续的能力超过茜素红S,表明Alen-Cds具有针对性药物递送的潜力,并在体内调查中提供额外的动机。据我们所知,这是第一个体外,前体内,以及直接骨骼靶向交付的体内演示,支持使用荧光CD在治疗各种骨疾病,如骨质疏松症,Paget疾病和转移性骨癌。

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  • 来源
    《RSC Advances》 |2019年第5期|共10页
  • 作者单位

    KRIBB Hazards Monitoring BNT Res Ctr Daejeon 34141 South Korea;

    KRIBB Dis Target Struct Res Ctr Daejeon 34141 South Korea;

    Chonnam Natl Univ Dept Polymer Engn Gwangju 61186 South Korea;

    KRIBB Hazards Monitoring BNT Res Ctr Daejeon 34141 South Korea;

    UST Dept Biotechnol Daejeon 34113 South Korea;

    UST Dept Biotechnol Daejeon 34113 South Korea;

    KRIBB Dis Target Struct Res Ctr Daejeon 34141 South Korea;

    KRIBB Hazards Monitoring BNT Res Ctr Daejeon 34141 South Korea;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 化学;
  • 关键词

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