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Gene Expression-Based Identification of Antigen-Responsive CD8+ T Cells on a Single-Cell Level.


ABSTRACT: CD8+ T cells are important effectors of adaptive immunity against pathogens, tumors, and self antigens. Here, we asked how human cognate antigen-responsive CD8+ T cells and their receptors could be identified in unselected single-cell gene expression data. Single-cell RNA sequencing and qPCR of dye-labeled antigen-specific cells identified large gene sets that were congruently up- or downregulated in virus-responsive CD8+ T cells under different antigen presentation conditions. Combined expression of TNFRSF9, XCL1, XCL2, and CRTAM was the most distinct marker of virus-responsive cells on a single-cell level. Using transcriptomic data, we developed a machine learning-based classifier that provides sensitive and specific detection of virus-responsive CD8+ T cells from unselected populations. Gene response profiles of CD8+ T cells specific for the autoantigen islet-specific glucose-6-phosphatase catalytic subunit-related protein differed markedly from virus-specific cells. These findings provide single-cell gene expression parameters for comprehensive identification of rare antigen-responsive cells and T cell receptors.

SUBMITTER: Fuchs YF 

PROVIDER: S-EPMC6851025 | biostudies-literature | 2019

REPOSITORIES: biostudies-literature

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Gene Expression-Based Identification of Antigen-Responsive CD8<sup>+</sup> T Cells on a Single-Cell Level.

Fuchs Yannick F YF   Sharma Virag V   Eugster Anne A   Kraus Gloria G   Morgenstern Robert R   Dahl Andreas A   Reinhardt Susanne S   Petzold Andreas A   Lindner Annett A   Löbel Doreen D   Bonifacio Ezio E  

Frontiers in immunology 20191106


CD8<sup>+</sup> T cells are important effectors of adaptive immunity against pathogens, tumors, and self antigens. Here, we asked how human cognate antigen-responsive CD8<sup>+</sup> T cells and their receptors could be identified in unselected single-cell gene expression data. Single-cell RNA sequencing and qPCR of dye-labeled antigen-specific cells identified large gene sets that were congruently up- or downregulated in virus-responsive CD8<sup>+</sup> T cells under different antigen presentat  ...[more]

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