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光热多光谱图像细胞计量术用于定量分析完整、染色和选择性燃烧组织中的纳米颗粒和微转移。

Photothermal multispectral image cytometry for quantitative histology of nanoparticles and micrometastasis in intact, stained and selectively burned tissues.

机构信息

Phillips Classic Laser and Nanomedicine Laboratories, University of Arkansas for Medical Sciences, Little Rock, Arkansas 72205, USA.

出版信息

Cytometry A. 2010 Nov;77(11):1049-58. doi: 10.1002/cyto.a.20977.

Abstract

There is a rapidly growing interest in the advanced analysis of histological data and the development of appropriate detection technologies in particular for mapping of nanoparticle distributions in tissue in nanomedicine applications. We evaluated photothermal (PT) scanning cytometry for color-coded imaging, spectral identification, and quantitative detection of individual nanoparticles and abnormal cells in histological samples with and without staining. Using this tool, individual carbon nanotubes, gold nanorods, and melanoma cells with intrinsic melanin markers were identified in unstained (e.g. sentinel lymph nodes) and conventionally-stained tissues. In addition, we introduced a spectral burning technique for histology through selective laser bleaching areas with nondesired absorption background and nanobubble-based PT signal amplification. The obtained data demonstrated the promise of PT cytometry in the analysis of low-absorption samples and mapping of various individual nanoparticles' distribution that would be impossible with existing assays. Comparison of PT cytometry and photoacoustic (PA) cytometry previously developed by us, revealed that these methods supplement each other with a sensitivity advantage (up to 10-fold) of contactless PT technique in assessment of thin (≤100 μm) histological samples, while PA imaging provides characterization of thicker samples which, however, requires an acoustic contact with transducers. A potential of high-speed integrated PT-PA cytometry for express histology and immunohistochemistry of both intact and stained heterogeneous tissues with high sensitivity at the zepromolar concentration level is further highlighted.

摘要

人们对组织学数据的高级分析以及特别是纳米医学应用中用于组织内纳米粒子分布映射的适当检测技术的开发越来越感兴趣。我们评估了光热(PT)扫描细胞术,用于对未经染色(例如前哨淋巴结)和常规染色组织中的单个纳米粒子和异常细胞进行彩色成像、光谱识别和定量检测。使用这种工具,可以识别未经染色(例如前哨淋巴结)和常规染色组织中的单个碳纳米管、金纳米棒和具有内在黑色素标记的黑色素瘤细胞。此外,我们通过选择性激光烧蚀具有不需要的吸收背景的区域并基于纳米气泡的 PT 信号放大,引入了一种用于组织学的光谱燃烧技术。获得的数据表明,PT 细胞术在分析低吸收样品和绘制各种单个纳米粒子分布方面具有很大的应用潜力,而现有的检测方法是无法实现的。PT 细胞术和我们之前开发的光声(PA)细胞术的比较表明,这些方法相互补充,接触式 PT 技术在评估≤100μm 的薄组织学样品时具有更高的灵敏度优势(高达 10 倍),而 PA 成像提供了对更厚样品的特征描述,但需要与换能器进行声学接触。进一步强调了高速集成的 PT-PA 细胞术在完整和染色的异质组织的快速组织学和免疫组织化学中的潜力,具有高灵敏度,在 zepromolar 浓度水平下。

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