Activation of MiR-21-Regulated Pathways in Immune Aging Selects Against Signatures Characteristic of Memory T Cells

Overview

Journal Cell Rep

Publisher Cell Press

Specialties Biology
Cell Biology
Molecular Biology

Date 2018 Nov 22

PMID 30463012

Citations 61

Authors

Chulwoo Kim

Bin Hu

Rohit R Jadhav

Jun Jin

Huimin Zhang

Mary M Cavanagh

Rama S Akondy

Rafi Ahmed

Cornelia M Weyand

Jorg J Goronzy

Affiliations

Soon will be listed here.

Abstract

Induction of protective vaccine responses, governed by the successful generation of antigen-specific antibodies and long-lived memory T cells, is increasingly impaired with age. Regulation of the T cell proteome by a dynamic network of microRNAs is crucial to T cell responses. Here, we show that activation-induced upregulation of miR-21 biases the transcriptome of differentiating T cells away from memory T cells and toward inflammatory effector T cells. Such a transcriptome bias is also characteristic of T cell responses in older individuals who have increased miR-21 expression and is reversed by antagonizing miR-21. miR-21 targets negative feedback circuits in several signaling pathways. The concerted, sustained activity of these signaling pathways in miR-21 T cells disfavors the induction of transcription factor networks involved in memory cell differentiation. Our data suggest that curbing miR-21 upregulation or activity in older individuals may improve their ability to mount effective vaccine responses.

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