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Systems pathology by multiplexed immunohistochemistry and whole-slide digital image analysis

机译:通过多重免疫组织化学和全幻灯片数字图像分析的系统病理学

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摘要

The paradigm of molecular histopathology is shifting from a single-marker immunohistochemistry towards multiplexed detection of markers to better understand the complex pathological processes. However, there are no systems allowing multiplexed IHC (mIHC) with high-resolution whole-slide tissue imaging and analysis, yet providing feasible throughput for routine use. We present an mIHC platform combining fluorescent and chromogenic staining with automated whole-slide imaging and integrated whole-slide image analysis, enabling simultaneous detection of six protein markers and nuclei, and automatic quantification and classification of hundreds of thousands of cells in situ in formalin-fixed paraffin-embedded tissues. In the first proof-of-concept, we detected immune cells at cell-level resolution (n = 128,894 cells) in human prostate cancer, and analysed T cell subpopulations in different tumour compartments (epithelium vs. stroma). In the second proof-of-concept, we demonstrated an automatic classification of epithelial cell populations (n = 83,558) and glands (benign vs. cancer) in prostate cancer with simultaneous analysis of androgen receptor (AR) and alpha-methylacyl-CoA (AMACR) expression at cell-level resolution. We conclude that the open-source combination of 8-plex mIHC detection, whole-slide image acquisition and analysis provides a robust tool allowing quantitative, spatially resolved whole-slide tissue cytometry directly in formalin-fixed human tumour tissues for improved characterization of histology and the tumour microenvironment.
机译:分子组织病理学的范式正在从单标记免疫组织化学转变为标记的多重检测,以更好地了解复杂的病理过程。但是,还没有系统可以对高分辨率的全玻片组织成像和分析进行多路复用的IHC(mIHC),却无法为常规使用提供通量。我们提供了一个mIHC平台,该平台将荧光和生色染色与自动全幻灯片成像和集成的全幻灯片图像分析相结合,能够同时检测六个蛋白质标记和细胞核,并在福尔马林中自动定量和分类数十万个细胞固定石蜡包埋的组织。在第一个概念验证中,我们在人前列腺癌中检测到了具有细胞水平分辨率的免疫细胞(n = 128,894个细胞),并分析了不同肿瘤区室(上皮与基质)中的T细胞亚群。在第二个概念验证中,我们证明了前列腺癌中上皮细胞群(n = 83,558)和腺体(良性与癌性)的自动分类,同时对雄激素受体(AR)和α-甲基酰基辅酶A( AMACR)表达式在单元格级别的分辨率。我们得出的结论是,将8重mIHC检测,全玻片图像采集和分析的开源组合提供了一个强大的工具,可直接在福尔马林固定的人类肿瘤组织中进行定量,空间分辨的全玻片组织细胞计数,以改善组织学特征和肿瘤微环境。

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