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Self-assembly of four generations of RNA dendrimers for drug shielding with controllable layer-by-layer release

机译:自组装的四代的RNA树枝状分子与可控药物屏蔽逐层释放

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摘要

Chemical dendrimers have been shown to be a promising drug delivery platform due to their advantageous properties such as monodispersity, multivalency and branched structure. Taking advantage of self-assembly and its intrinsic negative charge, we used RNA as the building block for dendrimer construction to eliminate complex synthesis procedures and cationic charge-related toxicity. Oligo ribonucleotides produced by solid phase chemical synthesis allow the large-scale manufacture of homologous RNA dendrimers. Employing concepts from RNA nanotechnology enabled the controllable production of dendrimers with generations from G(1), G(2), G(3), to G(4)with layer-by-layer release capability. The conjugation of functional groups into individual RNA strands and the incorporation of functionalized RNA strands into the dendrimers at different sites have been reported. Anticancer drugs loaded into RNA dendrimers showed comparable cancer cell inhibition effect to free drugs. Encapsulation of cell binding ligands and hydrophobic drugs within the dendrimer significantly reduced the efficiency of cell binding and protein binding respectively, demonstrating the shielding effect of RNA dendrimers. The results imply a potential application of RNA dendrimer for delivery, shielding and controlled release of hydrophobic drugsin vivo.
机译:化学聚合物已被证明是一个由于他们有前途的药物输送平台有利的单分散性等性能,多价和分支结构。自组装及其内在的优势负电荷,我们使用RNA的建筑阻止聚合物建设来消除复杂的合成过程和阳离子处理毒性。由固相化学合成同源RNA的大规模生产树枝状分子。纳米技术使可控树枝状分子的一代又一代的生产G (1), G (2), (3), G(4)分层技术释放能力。组织成单独的RNA链将功能化RNA链树枝状分子在不同的网站报道。树枝状分子显示类似的癌细胞免费药物抑制效果。细胞结合配体和疏水性药物聚合物明显减少了效率的细胞蛋白质绑定和绑定分别展示了屏蔽效果RNA的树枝状分子。核糖核酸聚合物的应用交付,保护和控制释放疏水drugsin活着。

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