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Imaging the uptake of gold nanoshells in live cells using plasmon resonance enhanced four wave mixing microscopy

机译:使用等离子体共振增强四波混合显微镜对活细胞中金纳米壳的摄取进行成像

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摘要

Gold nanoshells (GNS) are novel metal nanoparticles exhibiting attractive optical properties which make them highly suitable for biophotonics applications. We present a novel investigation using plasmon-enhanced four wave mixing microscopy combined with coherent anti-Stokes Raman scattering (CARS) microscopy to visualize the distribution of 75 nm radius GNS within live cells. During a laser tolerance study we found that cells containing nanoshells could be exposed to < 2.5 mJ each with no photo-thermally induced necrosis detected, while cell death was linearly proportional to the power over this threshold. The majority of the GNS signal detected was from plasmon-enhanced four wave mixing (FWM) that we detected in the epi-direction with the incident lasers tuned to the silent region of the Raman spectrum. The cellular GNS distribution was visualized by combining the epi-detected signal with forwards-detected CARS at the CH2 resonance. The applicability of this technique to real-world nanoparticle dosing problems was demonstrated in a study of the effect of H2S on nanoshell uptake using two donor molecules, NaHS and GYY4137. As GYY4137 concentration was increased from 10 μM to 1 mM, the nanoshell pixel percentage as a function of cell volume (PPCV) increased from 2.15% to 3.77%. As NaHS concentration was increased over the same range, the nanoshell PPCV decreased from 12.67% to 11.47%. The most important factor affecting uptake in this study was found to be the rate of H2S release, with rapid-release from NaHS resulting in significantly greater uptake.
机译:金纳米壳(GNS)是新型金属纳米颗粒,具有吸引人的光学特性,使其非常适合生物光子学应用。我们目前使用等离子体增强四波混合显微镜与相干抗斯托克斯拉曼散射(CARS)显微镜相结合,以可视化活细胞内75 nm半径GNS的分布,进行了一项新颖的研究。在激光耐受性研究中,我们发现含有纳米壳的细胞可以暴露于<2.5 mJ,且未检测到光热诱导的坏死,而细胞死亡与该阈值上的功率成线性比例。所检测到的大部分GNS信号来自于等离激元增强的四波混频(FWM),我们在外延方向上将入射激光调谐到拉曼光谱的无声区,从而检测到了这种现象。通过将Epi检测到的信号与CH2共振处的正向检测到的CARS相结合,可以看到细胞的GNS分布。使用两种供体分子NaHS和GYY4137对H2S对纳米壳吸收的影响进行了研究,证明了该技术对现实世界中纳米颗粒给药问题的适用性。随着GYY4137浓度从10μM增加到1 mM,纳米壳像素百分比作为细胞体积(PPCV)的函数从2.15%增加到3.77%。随着NaHS浓度在相同范围内增加,纳米壳PPCV从12.67%降至11.47%。在这项研究中,影响摄取的最重要因素是H2S释放的速率,NaHS的快速释放导致摄取明显增加。

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