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Spatially resolved transcriptomics reveals the architecture of the tumor-microenvironment interface

Miranda V. Hunter, Reuben Moncada, Joshua M. Weiss, Itai Yanai, Richard M. White

2021Nature Communications285 citationsDOIOpen Access PDF

Abstract

During tumor progression, cancer cells come into contact with various non-tumor cell types, but it is unclear how tumors adapt to these new environments. Here, we integrate spatially resolved transcriptomics, single-cell RNA-seq, and single-nucleus RNA-seq to characterize tumor-microenvironment interactions at the tumor boundary. Using a zebrafish model of melanoma, we identify a distinct "interface" cell state where the tumor contacts neighboring tissues. This interface is composed of specialized tumor and microenvironment cells that upregulate a common set of cilia genes, and cilia proteins are enriched only where the tumor contacts the microenvironment. Cilia gene expression is regulated by ETS-family transcription factors, which normally act to suppress cilia genes outside of the interface. A cilia-enriched interface is conserved in human patient samples, suggesting it is a conserved feature of human melanoma. Our results demonstrate the power of spatially resolved transcriptomics in uncovering mechanisms that allow tumors to adapt to new environments.

Topics & Concepts

CiliumTumor microenvironmentTranscriptomeZebrafishBiologyCell biologyComputational biologyMelanomaCellCancerGeneGene expressionCancer researchGeneticsSingle-cell and spatial transcriptomicsCancer Genomics and DiagnosticsImmune cells in cancer