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Digital Switching of Local Arginine Density in a Genetically Encoded Self-Assembled Polypeptide Nanoparticle Controls Cellular Uptake

机译:遗传编码的自组装多肽纳米粒子中局部精氨酸密度的数字切换对照细胞摄取

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摘要

Cell-penetrating peptides (CPPs) are a class of molecules that enable efficient internalization of a wide variety of cargo in diverse cell types, making them desirable for delivery of anticancer drugs to solid tumors. For CPPs to be useful, it is important to be able to turn their function on in response to an external trigger that can be spatially localized in vivo. Here we describe an approach to turning on CPP function by modulation of the local density of arginine (Arg) residues by temperature-triggered micelle assembly of diblock copolymer elastin-like polypeptides (ELPBCs). A greater than 8-fold increase in cellular uptake occurs when Arg residues are presented on the corona of ELPBC micelles, as compared to the same ELPBC at a temperature in which it is a soluble unimer. This approach is the first to demonstrate digital `off-on' control of CPP activity by an extrinsic thermal trigger in a clinically relevant temperature range by modulation of the interfacial density of Arg residues on the exterior of a nanoparticle.
机译:细胞穿透肽(CPP)是一类分子,其能够在各种细胞类型中能够有效地内化各种货物,使其希望将抗癌药物递送至实体瘤。对于CPPS有用,重要的是能够响应于可以在体内空间地定位的外部触发器上的功能。在这里,我们描述了通过DIBlock共聚物弹性蛋白样多肽(ELPBCS)的温度触发的胶束组装来调制精氨酸(ARG)残留物的局部密度来打开CPP功能的方法。当在ELPBC胶束的电晕上呈现在ELPBC胶束上的Corna上时,会发生大于8倍的细胞摄取的增加,与其是可溶性单层的温度相同的ELPBC。通过在临床相关温度范围内通过调制纳米粒子外部的Arc残留物的界面密度来首先通过在临床相关温度范围内通过外部热触发来证明CPP活性的数字`OFF-OFF“。

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