The Antidepressant Mirtazapine Activates Hepatic Macrophages, Facilitating Pathogen Clearance While Limiting Tissue Damage in Mice

Rachelle Paige Davis; Wagdi Almishri; Craig Neal Jenne; Mark Gordon Swain

doi:10.3389/fimmu.2020.578654

The Antidepressant Mirtazapine Activates Hepatic Macrophages, Facilitating Pathogen Clearance While Limiting Tissue Damage in Mice

Front Immunol. 2020 Nov 3:11:578654. doi: 10.3389/fimmu.2020.578654. eCollection 2020.

Authors

Rachelle Paige Davis^{1

2}, Wagdi Almishri^{1

2}, Craig Neal Jenne^{1

2}, Mark Gordon Swain^{1

2}

Affiliations

¹ Department of Microbiology, Immunology, and Infectious Diseases, University of Calgary, Calgary, AB, Canada.
² Snyder Institute for Chronic Diseases, University of Calgary, Calgary, AB, Canada.

Abstract

Background and aims: Mirtazapine is an atypical antidepressant with antagonist activity for serotonin and histamine receptors. Clinical and experimental evidence suggests that, in addition to treating depression, mirtazapine also alters liver innate immunity and suppresses immune-driven hepatic macrophage activation. Liver macrophages, Kupffer cells, represent the largest collection of fixed macrophages in the body and are critical in regulating hepatic immunity. In addition to their capacity to regulate inflammation, Kupffer cells are key sentinels for clearing blood-borne pathogens, preventing their dissemination within the body. This process involves pathogen capture, phagocytosis, and activation-induced killing via reactive oxygen species (ROS) production. Therefore, we speculated that mirtazapine might adversely alter Kupffer cell pathogen-associated activation and killing.

Methods: Mice were treated with mirtazapine and time-dependent changes in Kupffer cells were characterized using intravital microscopy. Macrophage and neutrophil responses, bacterial dissemination, and liver damage were assessed following i.v. infection with a pathogenic strain of S. aureus.

Results: Mirtazapine rapidly (within 1.5 h) activates Kupffer cells, indicated by a loss of elongated shape with cellular rounding. However, this shape change did not result in impaired pathogen capture function, and, in fact, generated enhanced ROS production in response to S. aureus-induced sepsis. Neutrophil dynamics were altered with reduced cellular recruitment to the liver following infection. Bacterial dissemination post-intravenous administration was not altered by mirtazapine treatment; however, hepatic abscess formation was significantly reduced.

Conclusions: Mirtazapine rapidly activates Kupffer cells, associated with preserved bacterial capture functions and enhanced ROS generation capacity. Moreover, these changes in Kupffer cells were linked to a beneficial reduction in hepatic abscess size. In contrast to our initial speculation, mirtazapine may have beneficial effects in sepsis and warrants further exploration.

Keywords: imaging; infection; inflammation; liver; macrophage; mirtazapine.

Publication types

Research Support, Non-U.S. Gov't
Video-Audio Media

MeSH terms

Animals
Antidepressive Agents / pharmacology*
Disease Models, Animal
Host-Pathogen Interactions
Kupffer Cells / drug effects*
Kupffer Cells / metabolism
Kupffer Cells / microbiology
Liver / drug effects*
Liver / metabolism
Liver / microbiology
Liver / pathology
Liver Abscess / drug therapy*
Liver Abscess / metabolism
Liver Abscess / microbiology
Liver Abscess / pathology
Macrophage Activation / drug effects*
Mice, Inbred C57BL
Mirtazapine / pharmacology*
Neutrophil Infiltration / drug effects
Neutrophils / drug effects
Neutrophils / metabolism
Neutrophils / microbiology
Phagocytosis / drug effects*
Reactive Oxygen Species / metabolism
Staphylococcal Infections / drug therapy*
Staphylococcal Infections / metabolism
Staphylococcal Infections / microbiology
Staphylococcal Infections / pathology
Staphylococcus aureus / pathogenicity*
Time Factors

Substances

Antidepressive Agents
Reactive Oxygen Species
Mirtazapine