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Terminal PEGylated DNA-Gold Nanoparticle Conjugates Offering High Resistance to Nuclease Degradation and Efficient Intracellular Delivery of DNA Binding Agents

机译:末端pEG化的DNa-金纳米粒子缀合物提供高抗核酸酶降解和DNa结合剂的有效细胞内递送

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摘要

Over the past 10 years, polyvalent DNA–gold nanoparticle (DNA–GNP) conjugate has been demonstrated as an efficient, universal nanocarrier for drug and gene delivery with high uptake by over 50 different types of primary and cancer cell lines. A barrier limiting its in vivo effectiveness is limited resistance to nuclease degradation and nonspecific interaction with blood serum contents. Herein we show that terminal PEGylation of the complementary DNA strand hybridized to a polyvalent DNA–GNP conjugate can eliminate nonspecific adsorption of serum proteins and greatly increases its resistance against DNase I-based degradation. The PEGylated DNA–GNP conjugate still retains a high cell uptake property, making it an attractive intracellular delivery nanocarrier for DNA binding reagents. We show that it can be used for successful intracellular delivery of doxorubicin, a widely used clinical cancer chemotherapeutic drug. Moreover, it can be used for efficient delivery of some cell-membrane-impermeable reagents such as propidium iodide (a DNA intercalating fluorescent dye currently limited to the use of staining dead cells only) and a diruthenium complex (a DNA groove binder), for successful staining of live cells.
机译:在过去的十年中,多价DNA-金纳米颗粒(DNA-GNP)共轭物已被证明是一种有效的通用纳米载体,用于药物和基因的递送,被50多种不同类型的原代和癌细胞系高吸收。限制其体内效力的障碍是对核酸酶降解的抗性以及与血清含量的非特异性相互作用的有限。在本文中,我们显示了与多价DNA-GNP共轭物杂交的互补DNA链的末端PEG化可以消除血清蛋白的非特异性吸附,并大大提高了其对基于DNase I的降解的抵抗力。聚乙二醇化的DNA-GNP共轭物仍保留了高细胞摄取特性,使其成为DNA结合试剂的诱人细胞内递送纳米载体。我们显示它可以用于成功的细胞内递送阿霉素,一种广泛使用的临床癌症化疗药物。此外,它还可用于有效递送某些细胞膜不可渗透的试剂,例如碘化丙啶(一种目前仅限于使用染色死细胞的DNA嵌入荧光染料)和一种钌络合物(一种DNA凹槽结合剂),用于活细胞成功染色。

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