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Literature DB >> 28930685

Human Tissue-Resident Memory T Cells Are Defined by Core Transcriptional and Functional Signatures in Lymphoid and Mucosal Sites.

Brahma V Kumar¹, Wenji Ma², Michelle Miron³, Tomer Granot¹, Rebecca S Guyer¹, Dustin J Carpenter⁴, Takashi Senda¹, Xiaoyun Sun², Siu-Hong Ho¹, Harvey Lerner⁵, Amy L Friedman⁵, Yufeng Shen², Donna L Farber⁶.

Abstract

Tissue-resident memory T cells (TRMs) in mice mediate optimal protective immunity to infection and vaccination, while in humans, the existence and properties of TRMs remain unclear. Here, we use a unique human tissue resource to determine whether human tissue memory T cells constitute a distinct subset in diverse mucosal and lymphoid tissues. We identify a core transcriptional profile within the CD69+ subset of memory CD4+ and CD8+ T cells in lung and spleen that is distinct from that of CD69- TEM cells in tissues and circulation and defines human TRMs based on homology to the transcriptional profile of mouse CD8+ TRMs. Human TRMs in diverse sites exhibit increased expression of adhesion and inhibitory molecules, produce both pro-inflammatory and regulatory cytokines, and have reduced turnover compared with circulating TEM, suggesting unique adaptations for in situ immunity. Together, our results provide a unifying signature for human TRM and a blueprint for designing tissue-targeted immunotherapies.

Entities: Chemical

Keywords: RNA-seq; human immunology; memory T cells; mucosal immunity

Mesh：

Substances：

Year: 2017 PMID： 28930685 PMCID： PMC5646692 DOI： 10.1016/j.celrep.2017.08.078

Source DB: PubMed Journal: Cell Rep Impact factor: 9.995

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