AUTHOR=Moreira Jôsimar D. , Koch Bjørn E. V. , van Veen Suzanne , Walburg Kimberley V. , Vrieling Frank , Mara Pinto Dabés Guimarães Tânia , Meijer Annemarie H. , Spaink Herman P. , Ottenhoff Tom H. M. , Haks Mariëlle C. , Heemskerk Matthias T. 

TITLE=Functional Inhibition of Host Histone Deacetylases (HDACs) Enhances in vitro and in vivo Anti-mycobacterial Activity in Human Macrophages and in Zebrafish

JOURNAL=Frontiers in Immunology

VOLUME=11

YEAR=2020

URL=https://www.frontiersin.org/journals/immunology/articles/10.3389/fimmu.2020.00036

DOI=10.3389/fimmu.2020.00036

ISSN=1664-3224

ABSTRACT=<p>The rapid and persistent increase of drug-resistant <italic>Mycobacterium tuberculosis</italic> (<italic>Mtb</italic>) infections poses increasing global problems in combatting tuberculosis (TB), prompting for the development of alternative strategies including host-directed therapy (HDT). Since <italic>Mtb</italic> is an intracellular pathogen with a remarkable ability to manipulate host intracellular signaling pathways to escape from host defense, pharmacological reprogramming of the immune system represents a novel, potentially powerful therapeutic strategy that should be effective also against drug-resistant <italic>Mtb</italic>. Here, we found that host-pathogen interactions in <italic>Mtb</italic>-infected primary human macrophages affected host epigenetic features by modifying histone deacetylase (HDAC) transcriptomic levels. In addition, broad spectrum inhibition of HDACs enhanced the antimicrobial response of both pro-inflammatory macrophages (Mϕ1) and anti-inflammatory macrophages (Mϕ2), while selective inhibition of class IIa HDACs mainly decreased bacterial outgrowth in Mϕ2. Moreover, chemical inhibition of HDAC activity during differentiation polarized macrophages into a more bactericidal phenotype with a concomitant decrease in the secretion levels of inflammatory cytokines. Importantly, <italic>in vivo</italic> chemical inhibition of HDAC activity in <italic>Mycobacterium marinum</italic>-infected zebrafish embryos, a well-characterized animal model for tuberculosis, significantly reduced mycobacterial burden, validating our <italic>in vitro</italic> findings in primary human macrophages. Collectively, these data identify HDACs as druggable host targets for HDT against intracellular <italic>Mtb</italic>.</p>