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Tissue Dynamics Spectroscopy for Three-Dimensional Tissue-Based Drug Screening

机译:组织动力学光谱用于基于三维组织的药物筛选

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Tissue dynamics spectroscopy combines dynamic light scattering with short-coherence digital holography to capture intracellular motion inside multicellular tumor spheroid tissue models. The cellular mechanical activity becomes an endogenous imaging contrast agent for motility contrast imaging. Fluctuation spectroscopy is performed on dynamic speckle from the proliferating shell and hypoxic core to generate drug - response spectrograms that are frequency versus time representations of the changes in spectral content induced by an applied compound or an environmental perturbation. A combination of 28 reference compounds and conditions applied to rat osteogenic UMR-106 spheroids generated spectrograms that were crosscorrelated in a similarity matrix used for unsupervised hierarchical clustering of similar compound responses. This work establishes the feasibility of tissue dynamics spectroscopy for three-dimensional tissue-based phenotypic profiling of drug response as a fully endogenous probe of the response of tissue to reference compounds.
机译:组织动力学光谱将动态光散射与短相干数字全息技术相结合,以捕获多细胞肿瘤球体组织模型内部的细胞内运动。细胞的机械活性成为运动性造影成像的内源性成像造影剂。对来自扩散壳和低氧核的动态散斑进行波动光谱分析,以生成药物反应光谱图,该光谱图是由使用的化合物或环境扰动引起的光谱含量变化的频率对时间的表示。 28种参考化合物和应用于大鼠成骨UMR-106球体的条件的组合产生了在相似矩阵中互相关的光谱图,该相似矩阵用于相似化合物响应的无监督分层聚类。这项工作建立了基于三维动力学的药物反应作为组织对参考化合物反应的完全内源性探针的基于表型的三维表型分析的组织动力学光谱学的可行性。

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