Lymphocyte innateness defined by transcriptional states reflects a balance between proliferation and effector functions

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2019-02-08
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English
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Springer Nature
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Abstract

How innate T cells (ITC), including invariant natural killer T (iNKT) cells, mucosal-associated invariant T (MAIT) cells, and γδ T cells, maintain a poised effector state has been unclear. Here we address this question using low-input and single-cell RNA-seq of human lymphocyte populations. Unbiased transcriptomic analyses uncover a continuous ‘innateness gradient’, with adaptive T cells at one end, followed by MAIT, iNKT, γδ T and natural killer cells at the other end. Single-cell RNA-seq reveals four broad states of innateness, and heterogeneity within canonical innate and adaptive populations. Transcriptional and functional data show that innateness is characterized by pre-formed mRNA encoding effector functions, but impaired proliferation marked by decreased baseline expression of ribosomal genes. Together, our data shed new light on the poised state of ITC, in which innateness is defined by a transcriptionally-orchestrated trade-off between rapid cell growth and rapid effector function.

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Gutierrez-Arcelus, M., Teslovich, N., Mola, A.R. et al. Lymphocyte innateness defined by transcriptional states reflects a balance between proliferation and effector functions. Nat Commun 10, 687 (2019). https://doi.org/10.1038/s41467-019-08604-4
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2041-1723
2041-1723
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Supported by the National Institutes of Health (AI102945 to P.J.B., AI113046 and AI063428 to M.B.B., U19AI111224, U01GM092691, U01HG009379, and R01AR063759 to S.R.), the Doris Duke Charitable Foundation (2013097 to S.R.), the Violin and Karol families (to P.J.B.), and the Swiss National Science Foundation (Early Postdoc Mobility Fellowship to M.G.-A.).
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Nature Communications
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