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Water soluble nanoporous nanoparticle for in vivo targeted drug delivery and controlled release in B cells tumor context

机译:水溶性纳米多孔纳米颗粒,用于体内靶向药物输送和在B细胞肿瘤环境中受控释放

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摘要

Multitasking nanoparticles are gaining great attention for smart drug delivery systems. The exploration of the nano-scale opens new concrete opportunities for revealing new properties and undiscovered cell-particle interactions. Here we present a biodegradable nanoporous silicon nanoparticle that can be successfully employed for in vivo targeted drug delivery and sustained release. The bare nanoporous nanocarriers can be accurately designed and fabricated with an effective control of porosity, surface chemistry and particle size, up to a few nm. The proposed nanoparticles exhibit several remarkable features including high payload, biodegradability, no toxicity, and multiple loading in water without the need of additional chemical reagents at room temperature. The targeting strategy is based on phage display technology that was successfully used to discover cell surface binding peptide for murine B lymphoma A20 cell line. The peptide used in combination with the nanoporous nanoparticles allows an efficient in vivo targeting, a sustained release and a sensible therapeutic effect.
机译:多任务纳米颗粒对智能药物输送系统引起了极大的关注。对纳米级的探索为揭示新特性和未发现的细胞粒子相互作用开辟了新的具体机会。在这里,我们提出了可生物降解的纳米多孔硅纳米颗粒,该纳米颗粒可以成功用于体内靶向药物递送和持续释放。裸纳米多孔纳米载体可以通过有效控制孔隙度,表面化学和粒度的有效控制和制造。所提出的纳米颗粒表现出几种显着的特征,包括高有效载荷,可生物降解性,无毒性以及在室温下需要额外的化学试剂的水中多重负载。靶向策略基于噬菌体显示技术,该技术成功地用于发现鼠B淋巴瘤A20细胞系的细胞表面结合肽。与纳米多孔纳米颗粒结合使用的肽可有效地体内靶向,持续释放和明智的治疗作用。

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