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Design of a Functionalized Metal-Organic Framework System for Enhanced Targeted Delivery to Mitochondria

机译:功能性金属有机框架系统的设计,以增强针对性地向线粒体的靶向递送。

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Mitochondria play a key role in oncogenesis and constitute one of the most important targets for cancer treatments. Although the most effective way to deliver drugs to mitochondria is by covalently linking them to a lipophilic cation, the in vivo delivery of free drugs still constitutes a critical bottleneck. Herein, we report the design of a mitochondria-targeted metal-organic framework (MOF) that greatly increases the efficacy of a model cancer drug, reducing the required dose to less than 1% compared to the free drug and ca. 10% compared to the nontargeted MOF. The performance of the system is evaluated using a holistic approach ranging from microscopy to transcriptomics. Super-resolution microscopy of MCF-7 cells treated with the targeted MOF system reveals important mitochondrial morphology changes that are clearly associated with cell death as soon as 30 min after incubation. Whole transcriptome analysis of cells indicates widespread changes in gene expression when treated with the MOF system, specifically in biological processes that have a profound effect on cell physiology and that are related to cell death. We show how targeting MOFs toward mitochondria represents a valuable strategy for the development of new drug delivery systems.
机译:线粒体在肿瘤发生中起关键作用,并构成癌症治疗的最重要靶标之一。尽管将药物传递至线粒体的最有效方法是将其与亲脂性阳离子共价连接,但体内游离药物的传递仍构成关键瓶颈。在本文中,我们报告了针对线粒体的金属有机框架(MOF)的设计,该框架极大地提高了模型癌症药物的功效,与游离药物和ca相比,所需剂量减少至小于1%。与非目标MOF相比,为10%。使用从显微镜到转录组学的整体方法评估系统的性能。靶向MOF系统处理的MCF-7细胞的超高分辨率显微镜检查显示,重要的线粒体形态变化与孵育后30分钟之内的细胞死亡显然相关。对细胞进行全转录组分析表明,当用MOF系统处理时,尤其是在对细胞生理产生深远影响并与细胞死亡有关的生物学过程中,基因表达发生了广泛变化。我们展示了将MOF靶向线粒体是如何代表开发新药物递送系统的宝贵策略。

著录项

  • 来源
    《Journal of the American Chemical Society》 |2020年第14期|6661-6674|共14页
  • 作者单位

    Adsorption & Advanced Materials Laboratory (AAML) Department of Chemical Engineering & Biotechnology University of Cambridge Cambridge CB3 0AS U.K.;

    WestCHEM School of Chemistry University of Glasgow Glasgow G12 8QQ U.K.;

    Laser Analytics Group Department of Chemical Engineering & Biotechnology University of Cambridge Cambridge CB3 0AS UK;

    Cambridge Infinitus Research Centre Department of Chemical Engineering & Biotechnology University of Cambridge Cambridge CB3 OAS U.K;

    Laboratorio de Materiales Avanzados Departamento de Quimica Inorganica-Instituto Universitario de Materiales Universidad de Alicante E-03690 San Vicente del Raspeig Spain;

    Molecular Neuroscience Group Department of Chemical Engineering & Biotechnology University of Cambridge Cambridge CB3 0AS U.K.;

    Laser Analytics Group Department of Chemical Engineering & Biotechnology University of Cambridge Cambridge CB3 0AS U.K.;

  • 收录信息 美国《科学引文索引》(SCI);美国《工程索引》(EI);美国《生物学医学文摘》(MEDLINE);美国《化学文摘》(CA);
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

  • 入库时间 2022-08-18 05:28:35

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