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Single-cell transcriptomic analysis of mIHC images via antigen mapping

机译:通过抗原映射MIHC图像的单细胞转录组分析

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Highly multiplexed immunohistochemistry (mIHC) enables the staining and quantification of dozens of antigens in a tissue section with single-cell resolution. However, annotating cell populations that differ little in the profiled antigens or for which the antibody panel does not include specific markers is challenging. To overcome this obstacle, we have developed an approach for enriching mIHC images with single-cell RNA sequencing data, building upon recent experimental procedures for augmenting single-cell transcriptomes with concurrent antigen measurements. Spatially-resolved Transcriptomics via Epitope Anchoring (STvEA) performs transcriptome-guided annotation of highly multiplexed cytometry datasets. It increases the level of detail in histological analyses by enabling the systematic annotation of nuanced cell populations, spatial patterns of transcription, and interactions between cell types. We demonstrate the utility of STvEA by uncovering the architecture of poorly characterized cell types in the murine spleen using published cytometry and mIHC data of this organ.
机译:高度复用免疫组织化学(MIHC)使得在具有单细胞分辨率的组织部分中的数十种抗原染色和定量。然而,在异形抗原或抗体面板不包括特定标记的抗体或其抗体面板不包括特定标记的注释细胞群是挑战性的。为了克服这种障碍,我们开发了一种用单细胞RNA测序数据来富集MIHC图像的方法,在最近的实验过程中建立具有同时抗原测量的单细胞转录om。通过表位锚定(STVEA)的空间分辨的转录组织进行了高度复用细胞计数数据集的转录组导向注释。通过使细胞群体,转录的空间模式和细胞类型之间的相互作用来增加组织学分析中的细节水平。我们通过使用公开的细胞测定法和该器官的MIHC数据揭示鼠脾脏中表征较差的细胞类型的体系结构来证明STVEA的效用。

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