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Optimizing the properties of the protein corona surrounding nanoparticles for tuning payload release

机译:优化纳米粒子周围蛋白电晕的性质以调节有效负载释放

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摘要

We manipulate the passive release rates of DNA payloads on protein coronas formed around nanoparticles (NPs) by varying the corona composition. The coronas are prepared using a mixture of hard and soft corona proteins. We form coronas around gold nanorods (NRs), nanobones (NBs), and carbon nanotubes (CNTs) from human serum (HS) and find that tuning the amount of human serum albumin (HSA) in the NR-coronas (NR-HS-DNA) changes the payload release profile. The effect of buffer strength, HS concentration, and concentration of the cetyltrimethylammonium bromide (CTAB) passivating the NP surfaces on passive release is explored. We find that corona properties play an important role in passive release, and concentrations of CTAB, HS, and phosphate buffer used in corona formation can tune payload release profiles. These advances in understanding protein corona properties bring us closer toward developing a set of basic design rules that enable their manipulation and optimization for particular biological applications.
机译:我们通过改变电晕的组成来控制在纳米粒子(NPs)周围形成的蛋白质电晕上DNA负载的被动释放速率。使用硬和软电晕蛋白的混合物制备电晕。我们在人血清(HS)中的金纳米棒(NRs),纳米骨(NBs)和碳纳米管(CNTs)周围形成电晕,并发现调整NR电晕(NR-HS-中的人血清白蛋白(HSA)的量DNA)更改有效负载释放配置文件。探索了缓冲剂强度,HS浓度和十六烷基三甲基溴化十六烷基铵(CTAB)钝化NP表面对被动释放的影响。我们发现电晕特性在被动释放中起着重要作用,并且用于电晕形成的CTAB,HS和磷酸盐缓冲液的浓度可以调节有效负载的释放曲线。在了解蛋白质电晕特性方面的这些进展使我们更加接近于开发一套基本设计规则,从而使其能够针对特定的生物学应用进行操纵和优化。

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