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Graph deep learning for the characterization of tumour microenvironments from spatial protein profiles in tissue specimens. | LitMetric

AI Article Synopsis

  • Multiplexed immunofluorescence imaging enables detailed molecular profiling of cellular environments, but analyzing the intricate data for disease-related patterns is complex.
  • The study introduces a graph neural network that models tumor microenvironments using spatial protein profiles, effectively capturing unique cellular interactions linked to clinical outcomes.
  • This approach demonstrated superior accuracy in predicting patient outcomes for head-and-neck and colorectal cancers compared to traditional spatial analysis methods, offering valuable insights into tumor cell organization and its impact on prognosis.

Article Abstract

Multiplexed immunofluorescence imaging allows the multidimensional molecular profiling of cellular environments at subcellular resolution. However, identifying and characterizing disease-relevant microenvironments from these rich datasets is challenging. Here we show that a graph neural network that leverages spatial protein profiles in tissue specimens to model tumour microenvironments as local subgraphs captures distinctive cellular interactions associated with differential clinical outcomes. We applied this spatial cellular-graph strategy to specimens of human head-and-neck and colorectal cancers assayed with 40-plex immunofluorescence imaging to identify spatial motifs associated with cancer recurrence and with patient survival after treatment. The graph deep learning model was substantially more accurate in predicting patient outcomes than deep learning approaches that model spatial data on the basis of the local composition of cell types, and it generated insights into the effect of the spatial compartmentalization of tumour cells and granulocytes on patient prognosis. Local graphs may also aid in the analysis of disease-relevant motifs in histology samples characterized via spatial transcriptomics and other -omics techniques.

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Source
http://dx.doi.org/10.1038/s41551-022-00951-wDOI Listing

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