Single-cell transcriptomics identifies an effectorness gradient shaping the response of CD4+ T cells to cytokines

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作者
Eddie Cano-Gamez
Blagoje Soskic
Theodoros I. Roumeliotis
Ernest So
Deborah J. Smyth
Marta Baldrighi
David Willé
Nikolina Nakic
Jorge Esparza-Gordillo
Christopher G. C. Larminie
Paola G. Bronson
David F. Tough
Wendy C. Rowan
Jyoti S. Choudhary
Gosia Trynka
机构
[1] Wellcome Genome Campus,Wellcome Sanger Institute
[2] Wellcome Genome Campus,Open Targets
[3] The Institute of Cancer Research,Functional Proteomics
[4] GSK R&D,Biostatistics
[5] GSK R&D,Functional Genomics, Medicinal Science and Technology
[6] GSK R&D,Human Genetics
[7] R&D Translational Biology,Human Target Validation Core
[8] Biogen,Adaptive Immunity RU
[9] GSK R&D,Novel Human Genetics
[10] GSK R&D,undefined
来源
Nature Communications | / 11卷
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摘要
Naïve CD4+ T cells coordinate the immune response by acquiring an effector phenotype in response to cytokines. However, the cytokine responses in memory T cells remain largely understudied. Here we use quantitative proteomics, bulk RNA-seq, and single-cell RNA-seq of over 40,000 human naïve and memory CD4+ T cells to show that responses to cytokines differ substantially between these cell types. Memory T cells are unable to differentiate into the Th2 phenotype, and acquire a Th17-like phenotype in response to iTreg polarization. Single-cell analyses show that T cells constitute a transcriptional continuum that progresses from naïve to central and effector memory T cells, forming an effectorness gradient accompanied by an increase in the expression of chemokines and cytokines. Finally, we show that T cell activation and cytokine responses are influenced by the effectorness gradient. Our results illustrate the heterogeneity of T cell responses, furthering our understanding of inflammation.
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