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Ionizable amphiphilic dendrimer-based nanomaterials with alkyl chain-substituted amines for tunable siRNA delivery to the liver endothelium in vivo

机译:具有烷基链取代胺的可电离的两亲树状聚合物纳米材料可在体内将siRNA可调地传递到肝内皮

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摘要

A library of dendrimers was synthesized and optimized for targeted small interfering RNA (siRNA) delivery to different cell subpopulations within the liver. Using a combinatorial approach, a library of these nanoparticle-forming materials was produced wherein the free amines on multigenerational poly(amido amine) and poly(propylenimine) dendrimers were substituted with alkyl chains of increasing length, and evaluated for their ability to deliver siRNA to liver cell subpopulations. Interestingly, two lead delivery materials could be formulated in a manner to alter their tissue tropism within the liver – with formulations from the same material capable of preferentially delivering siRNA to (i) endothelial cells, (ii) endothelial cells and hepatocytes, or (iii) endothelial cells, hepatocytes and tumor cells in vivo. The ability to broaden or narrow the cellular destination of siRNA within the liver may provide a useful tool to address a range of liver diseases.
机译:合成并优化了树枝状聚合物的文库,以将其靶向小干扰RNA(siRNA)递送至肝脏内的不同细胞亚群。使用组合方法,生成了这些纳米颗粒形成材料的库,其中多代聚(酰胺胺)和聚(丙二胺)树状聚合物上的游离胺被长度增加的烷基链取代,并评估了其将siRNA传递至肝细胞亚群。有趣的是,可以通过改变肝脏中组织趋向性的方式来配制两种铅递送材料-采用能够优先将siRNA递送至(i)内皮细胞,(ii)内皮细胞和肝细胞或(iii )体内的内皮细胞,肝细胞和肿瘤细胞。扩大或缩小肝脏中siRNA的细胞靶点的能力可能为解决一系列肝脏疾病提供有用的工具。

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