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首页> 外文期刊>ACS nano >DNA-gold nanoparticle reversible networks grown on cell surface marker sites: Application in diagnostics
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DNA-gold nanoparticle reversible networks grown on cell surface marker sites: Application in diagnostics

机译:细胞表面标记位点上生长的DNA-金纳米粒子可逆网络:在诊断中的应用

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摘要

Effective identification of breast cancer stem cells (CSC) benefits from a multiplexed approach to detect cell surface markers that can distinguish this subpopulation, which can invade and proliferate at sites of metastasis. We present a new approach for dual-mode sensing based on targeting using pointer and signal enhancement using enhancer particle networks for detection by surface plasmon resonance (SPR) and surface-enhanced Raman scattering (SERS). We demonstrate our concept to detect cell surface markers, CD44 and CD24, in three breast cancer cell lines to identify a CD44~+/CD24~- subpopulation of CSCs. The designed network structure can be well-controlled and has improved sensitivity compared to conventional approaches with ability to detect a single target on the membrane of a living cell. We have also developed a fractal approach to model the dimension of the network structure and developed an empirical relationship to estimate the number of particles in the network and its size. The empirical equation was validated with experiments and finite-difference time-domain simulations, and the cell phenotyping results were found to be in good agreement with published data from conventional sorting by flow cytometry.
机译:有效识别乳腺癌干细胞(CSC)得益于采用多种方法来检测可区分该亚群的细胞表面标志物,该亚群可以侵袭和扩散至转移部位。我们提出了一种新的双模式传感方法,该方法基于使用指针的目标定位和使用增强子粒子网络进行信号增强的表面等离子体激元共振(SPR)和表面增强拉曼散射(SERS)检测。我们展示了在三种乳腺癌细胞系中检测细胞表面标志物CD44和CD24的概念,以鉴定CSCs的CD44〜+ / CD24〜-亚群。与能够检测活细胞膜上单个靶标的常规方法相比,设计的网络结构可以得到很好的控制,并具有更高的灵敏度。我们还开发了一种分形方法来对网络结构的尺寸进行建模,并建立了一种经验关系来估计网络中粒子的数量及其大小。通过实验和有限差分时域仿真验证了该经验方程,并且发现细胞表型结果与通过流式细胞术从常规分选中公开的数据非常吻合。

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