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首页> 外文期刊>Journal of nanoscience and nanotechnology >Synergistic Nanomedicine: Passive, Active, and Ultrasound-Triggered Drug Delivery in Cancer Treatment
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Synergistic Nanomedicine: Passive, Active, and Ultrasound-Triggered Drug Delivery in Cancer Treatment

机译:协同纳米医学:被动,主动和超声触发的药物治疗癌症

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Nanocarriers are heavily researched as drug delivery vehicles capable of sequestering antineoplastic agents and then releasing their contents at the desired location. The feasibility of using such carriers stems from their ability to produce a multimodel delivery system whereby passive, ligand and triggered targeting can be applied in the fight against cancer. Passive targeting capitalizes on the leaky nature of tumor tissue which allows for the extravasation of particles with a size smaller than 0.5 mu m into the tumors. Ligand targeting utilizes the concept of receptor-mediated endocytosis and involves the conjugation of ligands onto the surface of nanoparticles, while triggered targeting involves the use of external and internal stimuli to release the carriers contents upon reaching the diseased location. In this review, micelles and liposomes have been considered due to the promising results they have shown in vivo and in vitro and their potential for advancements into clinical trials. Thus, this review focuses on the most recent advancements in the field of micellar and liposomal drug delivery and considers the synergistic effect of passive- and ligand-targeting strategies, and the use of ultrasound in triggering drug release at the tumor site.
机译:纳米载体已被广泛研究为能够隔离抗肿瘤药然后在所需位置释放其内含物的药物输送载体。使用这种载体的可行性源于它们产生多模型递送系统的能力,由此可以将被动,配体和触发靶向应用于抗癌。被动靶向利用肿瘤组织的渗漏性质,这允许将尺寸小于0.5微米的颗粒渗入肿瘤。配体靶向利用受体介导的内吞作用的概念,并且涉及配体在纳米颗粒表面上的缀合,而触发靶向涉及使用外部和内部刺激以在到达患病部位时释放载体内容物。在本综述中,由于胶束和脂质体在体内和体外显示出令人鼓舞的结果以及它们在临床试验中的发展潜力,因此已经考虑了它们。因此,本综述着眼于胶束和脂质体药物递送领域的最新进展,并考虑了被动靶向和配体靶向策略的协同作用,以及超声在触发肿瘤部位释放药物方面的应用。

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