首页> 美国卫生研究院文献>International Journal of Molecular Sciences >Photothermally Triggered Endosomal Escape and Its Influence on Transfection Efficiency of Gold-Functionalized JetPEI/pDNA Nanoparticles
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Photothermally Triggered Endosomal Escape and Its Influence on Transfection Efficiency of Gold-Functionalized JetPEI/pDNA Nanoparticles

机译:光热触发的内体逸出及其对金功能化JetPEI / pDNA纳米粒子转染效率的影响。

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摘要

Plasmonic nanoparticles for drug delivery have attracted increasing interest over the last few years. Their localized surface plasmon resonance causes photothermal effects on laser irradiation, which allows for delivering drugs in a spatio-temporally controlled manner. Here, we explore the use of gold nanoparticles (AuNP) as carriers for pDNA in combination with pulsed laser irradiation to induce endosomal escape, which is currently considered to be one of the major bottlenecks in macromolecular drug delivery on the intracellular level. In particular, we evaluate nanocomplexes composed of JetPEI (polyethylenimine)pDNA and 10 nm AuNP, which do not exhibit endosomal escape by themselves. After incubating HeLa cells with these complexes, we evaluated endosomal escape and transfection efficiency using low- and high-energy laser pulses. At low laser energy heat is produced by the nanocomplexes, while, at higher laser energy, explosive vapour nanobubbles (VNB) are formed. We investigated the ability of heat transfer and VNB formation to induce endosomal escape and we examine the integrity of pDNA cargo after inducing both photothermal effects. We conclude that JetPEI/pDNA/AuNP complexes are unable to induce meaningful transfection efficiencies because laser treatment causes either dysfunctionality of the cargo when VNB are formed or forms too small pores in the endosomal membrane to allow pDNA to escape in case of heating. We conclude that laser-induced VNB is the most suitable to induce effective pDNA endosomal escape, but a different nanocomplex structure will be required to keep the pDNA intact.
机译:在过去的几年中,用于药物递送的等离子纳米颗粒引起了越来越多的兴趣。它们的局部表面等离子体激元共振对激光辐照产生光热效应,从而可以以时空受控的方式传递药物。在这里,我们探讨了使用金纳米颗粒(AuNP)作为pDNA的载体与脉冲激光辐照诱导内体逃逸的结合,目前认为这是细胞内水平上大分子药物递送的主要瓶颈之一。特别是,我们评估了由JetPEI(聚乙烯亚胺)pDNA和10 nm AuNP组成的纳米复合物,它们自身并没有表现出内体逃逸。在将HeLa细胞与这些复合物孵育后,我们使用低能和高能激光脉冲评估了内体逃逸和转染效率。在低激光能量下,纳米复合物产生热量,而在高激光能量下,形成爆炸性蒸气纳米气泡(VNB)。我们研究了热传递和VNB形成诱导内体逃逸的能力,并在诱导了两种光热效应后检查了pDNA货物的完整性。我们得出的结论是,JetPEI / pDNA / AuNP复合物无法诱导有意义的转染效率,因为激光处理会导致在形成VNB时货物功能失调或在内体膜中形成过小的孔,从而在加热时无法使pDNA逸出。我们得出的结论是,激光诱导的VNB最适合诱导有效的pDNA内体逸出,但是需要不同的纳米复合物结构来保持pDNA完整。

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