Pro-inflammatory Cytokines Activate Hypoxia-inducible Factor 3α Via Epigenetic Changes in Mesenchymal Stromal/stem Cells

Overview

Journal Sci Rep

Specialty Science

Date 2018 Apr 13

PMID 29643458

Citations 18

Authors

Francesca Cuomo

Antonietta Coppola

Chiara Botti

Ciro Maione

Amalia Forte

Lucia Scisciola

Giuseppina Liguori

Ilaria Caiafa

Matilde Valeria Ursini

Umberto Galderisi

Marilena Cipollaro

Lucia Altucci

Gilda Cobellis

Affiliations

Soon will be listed here.

Abstract

Human mesenchymal stromal/stem cells (hMSCs) emerged as a promising therapeutic tool for ischemic disorders, due to their ability to regenerate damaged tissues, promote angiogenesis and reduce inflammation, leading to encouraging, but still limited results. The outcomes in clinical trials exploring hMSC therapy are influenced by low cell retention and survival in affected tissues, partially influenced by lesion's microenvironment, where low oxygen conditions (i.e. hypoxia) and inflammation coexist. Hypoxia and inflammation are pathophysiological stresses, sharing common activators, such as hypoxia-inducible factors (HIFs) and NF-κB. HIF1α and HIF2α respond essentially to hypoxia, activating pathways involved in tissue repair. Little is known about the regulation of HIF3α. Here we investigated the role of HIF3α in vitro and in vivo. Human MSCs expressed HIF3α, differentially regulated by pro-inflammatory cytokines in an oxygen-independent manner, a novel and still uncharacterized mechanism, where NF-κB is critical for its expression. We investigated if epigenetic modifications are involved in HIF3α expression by methylation-specific PCR and histone modifications. Robust hypermethylation of histone H3 was observed across HIF3A locus driven by pro-inflammatory cytokines. Experiments in a murine model of arteriotomy highlighted the activation of Hif3α expression in infiltrated inflammatory cells, suggesting a new role for Hif3α in inflammation in vivo.

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