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多孔硅及多孔硅固体脂质纳米复合材料用于被动靶向和成像的体内评估。

In vivo evaluation of porous silicon and porous silicon solid lipid nanocomposites for passive targeting and imaging.

作者信息

Kallinen Annukka M, Sarparanta Mirkka P, Liu Dongfei, Mäkilä Ermei M, Salonen Jarno J, Hirvonen Jouni T, Santos Hélder A, Airaksinen Anu J

机构信息

Laboratory of Radiochemistry, Department of Chemistry, University of Helsinki , FI-00014 Helsinki, Finland.

出版信息

Mol Pharm. 2014 Aug 4;11(8):2876-86. doi: 10.1021/mp500225b. Epub 2014 Jul 9.

Abstract

The use of nanoparticle carriers for the sustained release of cytotoxic drugs in cancer therapy can result in fewer adverse effects and can thus be of great benefit for the patient. Recently, a novel nanocomposite, prepared by the encapsulation of THCPSi nanoparticles within solid lipids (SLN), was developed and characterized as a promising drug delivery carrier in vitro. The present study describes the in vivo evaluation of unmodified THCPSi nanoparticles and THCPSi-solid lipid nanocomposites (THCPSi-SLNCs) as potential drug delivery carriers for cancer therapy by using (18)F radiolabeling for the detection of the particle biodistribution in mice. Passive tumor targeting of (18)F-THCPSis and (18)F-THCPSi-SLNCs by the enhanced permeation and retention effect was investigated in a murine breast cancer model. Encapsulation of THCPSi nanoparticles with solid lipids improved their accumulation in tumors at a 7 week time point (tumor-to-liver ratio 0.10 ± 0.08 and 0.24 ± 0.09% for (18)F-THCPSis and (18)F-THCPSi-SLNCs, respectively).

摘要

在癌症治疗中,使用纳米颗粒载体持续释放细胞毒性药物可减少不良反应,因此对患者大有裨益。最近,一种通过将THCPSi纳米颗粒包裹在固体脂质(SLN)中制备的新型纳米复合材料被开发出来,并在体外被表征为一种有前景的药物递送载体。本研究描述了通过使用(18)F放射性标记来检测小鼠体内颗粒生物分布,对未修饰的THCPSi纳米颗粒和THCPSi-固体脂质纳米复合材料(THCPSi-SLNCs)作为癌症治疗潜在药物递送载体的体内评估。在小鼠乳腺癌模型中研究了(18)F-THCPSis和(18)F-THCPSi-SLNCs通过增强渗透和滞留效应实现的被动肿瘤靶向。在7周时间点,用固体脂质包裹THCPSi纳米颗粒提高了它们在肿瘤中的蓄积((18)F-THCPSis和(18)F-THCPSi-SLNCs的肿瘤与肝脏比值分别为 0.10±0.08和0.24±0.09%)。

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