IFN-α Regulates Blimp-1 Expression Via MiR-23a and MiR-125b in Both Monocytes-derived DC and PDC

Overview

Journal PLoS One

Specialties General Medicine
Science

Date 2013 Aug 27

PMID 23977359

Citations 16

Authors

Stefania Parlato

Roberto Bruni

Paola Fragapane

Debora Salerno

Cinzia Marcantonio

Paola Borghi

Paola Tataseo

Anna Rita Ciccaglione

Carlo Presutti

Giulia Romagnoli

Irene Bozzoni

Filippo Belardelli

Lucia Gabriele

Affiliations

Soon will be listed here.

Abstract

Type I interferon (IFN-I) have emerged as crucial mediators of cellular signals controlling DC differentiation and function. Human DC differentiated from monocytes in the presence of IFN-α (IFN-α DC) show a partially mature phenotype and a special capability of stimulating CD4+ T cell and cross-priming CD8+ T cells. Likewise, plasmacytoid DC (pDC) are blood DC highly specialized in the production of IFN-α in response to viruses and other danger signals, whose functional features may be shaped by IFN-I. Here, we investigated the molecular mechanisms stimulated by IFN-α in driving human monocyte-derived DC differentiation and performed parallel studies on peripheral unstimulated and IFN-α-treated pDC. A specific miRNA signature was induced in IFN-α DC and selected miRNAs, among which miR-23a and miR-125b, proved to be negatively associated with up-modulation of Blimp-1 occurring during IFN-α-driven DC differentiation. Of note, monocyte-derived IFN-α DC and in vitro IFN-α-treated pDC shared a restricted pattern of miRNAs regulating Blimp-1 expression as well as some similar phenotypic, molecular and functional hallmarks, supporting the existence of a potential relationship between these DC populations. On the whole, these data uncover a new role of Blimp-1 in human DC differentiation driven by IFN-α and identify Blimp-1 as an IFN-α-mediated key regulator potentially accounting for shared functional features between IFN-α DC and pDC.

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