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Single File Flow of Biomimetic Beads for Continuous SERS Recording in a Microfluidic Device

机译:用于连续SERS记录在微流控设备中的仿生珠的单文件流

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A major challenge in cancer treatment is the quantification of biomarkers associated with a specific cancer type. Important biomarkers are the circulating tumor cells (CTCs) detached from the main cancer and circulating in the blood. CTCs are very rare and their identification is still an issue. Although CTCs quantification can be estimated by using fluorescent markers, all the fluorescence techniques are strongly limited by the number of emissions (therefore markers) that can be discriminated with one exciting line, by their bleaching characteristics, and by the intrinsic autofluorescence of biological samples. An emerging technique that can overcome these limitations is Surface Enhanced Raman Scattering (SERS). Signals of vibrational origin with intensity similar to those of fluorescence, but narrower bandwidths, can be easily discriminated even by exciting with a single laser line. We recently showed the benefit of this method with cells fixed on a surface. However, this approach is too demanding to be applied in clinical routine. To effectively increase the throughput of the SERS analysis, microfluidics represents a promising tool. We report two different hydrodynamic strategies, based on device geometry and liquids viscosity, to successfully combine a microfluidic design with SERS.
机译:癌症治疗中的主要挑战是与特定癌症类型相关的生物标记物的量化。重要的生物标志物是与主要癌症分离并在血液中循环的循环肿瘤细胞(CTC)。四氯化碳非常罕见,其识别仍然是一个问题。尽管可以使用荧光标记物估算四氯化碳的定量,但所有荧光技术都受到可通过一条激发线区分的发射数量(因此标记物),漂白特性以及生物样品固有的自发荧光的强烈限制。可以克服这些局限性的新兴技术是表面增强拉曼散射(SERS)。即使通过单条激光线激发,也可以轻松地区分具有类似于荧光的强度但带宽较窄的振动起源的信号。我们最近展示了将细胞固定在表面上这种方法的好处。但是,这种方法太过苛刻,无法应用于临床常规。为了有效地提高SERS分析的通量,微流体技术是一种很有前途的工具。我们根据设备的几何形状和液体粘度报告了两种不同的流体动力学策略,以成功地将微流体设计与SERS结合在一起。

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