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首页> 外文期刊>Applied Spectroscopy: Society for Applied Spectroscopy >Surface-Enhanced Raman Scattering Detection and Tracking of Nanoprobes: Enhanced Uptake and Nuclear Targeting in Single Cells
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Surface-Enhanced Raman Scattering Detection and Tracking of Nanoprobes: Enhanced Uptake and Nuclear Targeting in Single Cells

机译:纳米探针的表面增强拉曼散射检测和跟踪:单细胞中增强的摄取和核靶向。

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We describe the development and application of a co-functionalized nanoprobe and biodelivery platform combining a nuclear targeting peptide (NTP) for improved cellular uptake and intracellular targeting with p-mercaptobenzoic acid (pMBA) as a surface-enhanced Raman scattering (SERS) reporter for tracking and imaging. The nuclear targeting peptide, an HIV-1 protein-derived TAT sequence, has been previously shown to aid entry of cargo through the cell membrane via normal cellular processes, and furthermore, to localize small cargo to the nucleus of the cell. Previous work in our lab has verified cell uptake and distribution of the nanoprobes in clinically relevant mouse and human cell lines. In this work, two-dimensional SERS mapping was used to track the spatial and temporal progress of nanoparticle uptake in PC-3 human prostate cells and to characterize localization at various time points, demonstrating the potential for an intracellularly targeted multiplexed nanobiosensing system with excellent sensitivity and specificity. Silver nanoparticles co-functionalized with the TAT peptide showed greatly enhanced cellular uptake over the control nanoparticles lacking the targeting moiety. The ability to detect and monitor nanoprobe trafficking using SERS spectroscopy offers an improved alternative over previous tracking and detection methods such as light microscopy and fluorescence methods. The development of multifunctional nanoconstructs for intra-cellular delivery has potential clinical applications in early detection and selective treatment of disease in affected cells. Other applications include use in basic research aimed at understanding the inner workings of living cells and how they respond to chemical and biological stimuli.
机译:我们描述了共功能化纳米探针和生物传递平台的开发和应用,该平台结合了用于改善细胞摄取和胞内靶向的核靶向肽(NTP)与对巯基苯甲酸(pMBA)作为表面增强拉曼散射(SERS)报道分子跟踪和成像。先前已经显示,核靶向肽是HIV-1蛋白衍生的TAT序列,可通过正常的细胞过程帮助货物通过细胞膜进入,此外,还可将小货物定位在细胞核中。我们实验室以前的工作已经验证了临床相关的小鼠和人类细胞系中纳米探针的细胞摄取和分布。在这项工作中,二维SERS映射用于追踪PC-3人前列腺细胞中纳米颗粒吸收的空间和时间进展,并表征在不同时间点的定位,从而证明了具有出色灵敏度的细胞内靶向多重纳米生物传感系统的潜力和特异性。与TAT肽共功能化的银纳米颗粒比没有靶向部分的对照纳米颗粒显示出大大增强的细胞摄取。使用SERS光谱检测和监视纳米探针运输的能力提供了比以前的跟踪和检测方法(例如光学显微镜和荧光方法)更好的替代方法。用于细胞内递送的多功能纳米结构的开发在患病细胞的疾病的早期检测和选择性治疗中具有潜在的临床应用。其他应用包括在基础研究中使用,旨在了解活细胞的内部运作以及它们如何对化学和生物刺激作出反应。

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