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Semiautomated Multiplexed Quantum Dot-Based in Situ Hybridization and Spectral Deconvolution

机译:半自动基于量子点的原位杂交和光谱去卷积

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摘要

Gene expression profiling has identified several potentially useful gene signatures for predicting outcome or for selecting targeted therapy. However, these signatures have been developed in fresh or frozen tissue, and there is a need to apply them to routinely processed samples. Here, we demonstrate the feasibility of a potentially high-throughput methodology combining automated in situ hybridization with quantum dot-labeled oligonucleotide probes followed by spectral imaging for the detection and subsequent deconvolution of multiple signals. This method is semiautomated and quantitative and can be applied to formalin-fixed, paraffin-embedded tissues. We have combined dual in situ hybridization with immunohistochemistry, enabling simultaneous measurement of gene expression and cell lineage determination. The technique achieves levels of sensitivity and specificity sufficient for the potential application of known expression signatures to biopsy specimens in a semiquantitative way, and the semiautomated nature of the method enables application to high-throughput studies.
机译:基因表达谱已鉴定出几种潜在有用的基因特征,可用于预测结果或选择靶向治疗。然而,这些特征已经在新鲜或冷冻的组织中形成,并且需要将它们应用于常规处理的样品。在这里,我们证明了潜在的高通量方法论的可行性,该方法将自动原位杂交与量子点标记的寡核苷酸探针相结合,然后进行光谱成像以检测和随后对多个信号进行去卷积。该方法是半自动化的且定量的,可以应用于福尔马林固定,石蜡包埋的组织。我们将双重原位杂交与免疫组织化学相结合,可以同时测量基因表达和细胞谱系测定。该技术达到了足以将已知表达特征以半定量方式潜在地应用于活检标本的灵敏度和特异性水平,并且该方法的半自动化性质使其能够应用于高通量研究。

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