MicroRNA regulation in human CD8+ T cell subsets--cytokine exposure alone drives miR-146a expression

Hilary M Sheppard; Daniel Verdon; Anna E S Brooks; Vaughan Feisst; Yu-Yu Joyce Ho; Natalie Lorenz; Vicky Fan; Nigel P Birch; Alicia Didsbury; P Rod Dunbar

doi:10.1186/s12967-014-0292-0

MicroRNA regulation in human CD8+ T cell subsets--cytokine exposure alone drives miR-146a expression

J Transl Med. 2014 Oct 21:12:292. doi: 10.1186/s12967-014-0292-0.

Authors

Hilary M Sheppard^{1

2}, Daniel Verdon^{3

4}, Anna E S Brooks^{5

6}, Vaughan Feisst^{7

8}, Yu-Yu Joyce Ho^{9

10}, Natalie Lorenz¹¹, Vicky Fan¹², Nigel P Birch^{13

14}, Alicia Didsbury¹⁵, P Rod Dunbar^{16

17}

Affiliations

¹ School of Biological Sciences, University of Auckland, Thomas Building, Auckland, NZ, New Zealand. h.sheppard@auckland.ac.nz.
² Maurice Wilkins Centre for Molecular Biodiscovery, University of Auckland, Auckland, NZ, New Zealand. h.sheppard@auckland.ac.nz.
³ School of Biological Sciences, University of Auckland, Thomas Building, Auckland, NZ, New Zealand. dver013@aucklanduni.ac.nz.
⁴ Maurice Wilkins Centre for Molecular Biodiscovery, University of Auckland, Auckland, NZ, New Zealand. dver013@aucklanduni.ac.nz.
⁵ School of Biological Sciences, University of Auckland, Thomas Building, Auckland, NZ, New Zealand. a.brooks@auckland.ac.nz.
⁶ Maurice Wilkins Centre for Molecular Biodiscovery, University of Auckland, Auckland, NZ, New Zealand. a.brooks@auckland.ac.nz.
⁷ School of Biological Sciences, University of Auckland, Thomas Building, Auckland, NZ, New Zealand. v.feisst@auckland.ac.nz.
⁸ Maurice Wilkins Centre for Molecular Biodiscovery, University of Auckland, Auckland, NZ, New Zealand. v.feisst@auckland.ac.nz.
⁹ School of Biological Sciences, University of Auckland, Thomas Building, Auckland, NZ, New Zealand. yuyu.jh@gmail.com.
¹⁰ Maurice Wilkins Centre for Molecular Biodiscovery, University of Auckland, Auckland, NZ, New Zealand. yuyu.jh@gmail.com.
¹¹ School of Biological Sciences, University of Auckland, Thomas Building, Auckland, NZ, New Zealand. n.lorenz@auckland.ac.nz.
¹² Bioinformatics Institute, University of Auckland, Auckland, NZ, New Zealand. v.fan@auckland.ac.nz.
¹³ School of Biological Sciences, University of Auckland, Thomas Building, Auckland, NZ, New Zealand. n.birch@auckland.ac.nz.
¹⁴ Centre for Brain Research, University of Auckland, Auckland, NZ, New Zealand. n.birch@auckland.ac.nz.
¹⁵ School of Biological Sciences, University of Auckland, Thomas Building, Auckland, NZ, New Zealand. adid002@aucklanduni.ac.nz.
¹⁶ School of Biological Sciences, University of Auckland, Thomas Building, Auckland, NZ, New Zealand. r.dunbar@auckland.ac.nz.
¹⁷ Maurice Wilkins Centre for Molecular Biodiscovery, University of Auckland, Auckland, NZ, New Zealand. r.dunbar@auckland.ac.nz.

Abstract

Background: microRNAs (miRNAs) are emerging as key regulators of the immune system, but their role in CD8+ T cell differentiation is not well explored. Some evidence suggests that signals from cell surface receptors influence the expression of miRNAs in CD8+ T cells, and may have consequent effects on cell phenotype and function. We set out to investigate whether common gamma chain cytokines modulated human CD8+ T cell expression of miR-146a, which previous studies have associated with different stages of CD8+ differentiation. We also investigated how changes in miR-146a related to other miRNAs that alter with CD8+ differentiation status.

Methods: We treated human CD8+ T cells with the cytokines IL-2, IL-7 or IL-15 either at rest or after stimulation with anti-CD3 and anti-CD28. For some experiments we also purified human CD8+ T cell subsets ex vivo. Flow cytometry was used in parallel to assess cell surface memory marker expression. Total RNA from these cells was subjected to microarray analysis and real-time PCR for miRNA expression. Nucleofection studies were performed to assess potential mRNA targets of miR-146a.

Results: We find that miR-146a is up-regulated in naïve CD8+ T cells exposed to IL-2 or IL-15, even in the absence of an activating T cell receptor stimulus, but not when IL-7 is also present. miR-146a expression correlates with a memory phenotype in both ex vivo and in vitro cultured cells although in our hands overexpression of miR-146a was not sufficient alone to drive a full memory phenotype. In ex vivo analysis, miR-146a was one of a small number of miRNAs that was differentially expressed between naïve and memory CD8+ T cells.

Conclusions: miR-146a is emerging as a critical regulator of immune system. Our data shows that miR-146a expression is strongly influenced by the cytokine milieu even in the absence of a T cell receptor stimulus. Our results have implications for studies designed to assess the function of miR-146a, help to define a fingerprint of miRNA expression in CD8+ T cell subsets and may be useful when designing optimal protocols for T cell expansion as efficacy of T cell immunotherapy is correlated with an 'early' memory phenotype.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Antigens / metabolism
CD8-Positive T-Lymphocytes / drug effects
CD8-Positive T-Lymphocytes / metabolism*
Cytokines / pharmacology*
Fas-Associated Death Domain Protein / metabolism
Gene Expression Profiling
Gene Expression Regulation / drug effects*
Humans
Immunologic Memory
Interleukin-15 / pharmacology
Interleukin-2 / pharmacology
Interleukin-7 / pharmacology
MicroRNAs / genetics*
MicroRNAs / metabolism
Phenotype
Receptors, Antigen, T-Cell / metabolism
Receptors, CCR7 / metabolism
T-Lymphocyte Subsets / drug effects
T-Lymphocyte Subsets / metabolism*
TNF Receptor-Associated Factor 6 / metabolism
Up-Regulation / drug effects

Substances

Antigens
CCR7 protein, human
Cytokines
FADD protein, human
Fas-Associated Death Domain Protein
Interleukin-15
Interleukin-2
Interleukin-7
MIRN146 microRNA, human
MicroRNAs
Receptors, Antigen, T-Cell
Receptors, CCR7
TNF Receptor-Associated Factor 6