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On the design of precision nanomedicines

机译:关于精密纳米型ines的设计

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Tight control on the selectivity of nanoparticles’ interaction with biological systems is paramount for the development of targeted therapies. However, the large number of tunable parameters makes it difficult to identify optimal design “sweet spots” without guiding principles. Here, we combine superselectivity theory with soft matter physics into a unified theoretical framework and we prove its validity using blood brain barrier cells as target. We apply our approach to polymersomes functionalized with targeting ligands to identify the most selective combination of parameters in terms of particle size, brush length and density, as well as tether length, affinity, and ligand number. We show that the combination of multivalent interactions into multiplexed systems enable interaction as a function of the cell phenotype, that is, which receptors are expressed. We thus propose the design of a “bar-coding” targeting approach that can be tailor-made to unique cell populations enabling personalized therapies.
机译:对纳米颗粒与生物系统相互作用的选择性紧密控制对于靶向疗法的发展至关重要。然而,大量可调谐参数使得难以识别最佳设计“甜点”而不会引导原理。在这里,我们将柔软物理物理学结合到统一的理论框架中,我们将其使用血脑屏障细胞作为目标来证明其有效性。我们将方法应用于官能化配体官能化的聚合物,以识别粒度,刷子长度和密度的参数的最选择性组合,以及系绳长度,亲和力和配体数。我们表明,多重相互作用与多路复用系统的组合能够作为细胞表型的函数相互作用,即表达的受体。因此,我们提出了一种“条形码”靶向方法,可以定制到唯一的细胞群,从而实现个性化疗法。

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