Abstract

The herbal plant Angelica gigas (A. gigas) has been used in traditional medicine in East Asian countries, and its chemical components are reported to have many pharmacological effects. In this study, we showed that a bioactive ingredient of A. gigas modulates the functional activity of macrophages and investigated its effect on inflammation using a sepsis model. Among 12 different compounds derived from A. gigas, decursinol angelate (DA) was identified as the most effective in suppressing the induction of TNF-α and IL-6 in murine macrophages. When mice were infected with a lethal dose of methicillin-resistant Staphylococcus aureus (MRSA), DA treatment improved the mortality and bacteremia, and attenuated the cytokine storm, which was associated with decreased CD38+ macrophage populations in the blood and liver. In vitro studies revealed that DA inhibited the functional activation of macrophages in the expression of pro-inflammatory mediators in response to microbial infection, while promoting the bacterial killing ability with an increased production of reactive oxygen species. Mechanistically, DA treatment attenuated the NF-κB and Akt signaling pathways. Intriguingly, ectopic expression of an active mutant of IKK2 released the inhibition of TNF-α production by the DA treatment, whereas the inhibition of Akt resulted in enhanced ROS production. Taken together, our experimental evidence demonstrated that DA modulates the functional activities of pro-inflammatory macrophages and that DA could be a potential therapeutic agent in the management of sepsis.

Highlights

  • Upon pathogen infection, the innate immune system orchestrates an immediate early response to the invading microbe

  • The innate immunity against microbial infections is vital for the clearance of invading pathogens, which coincides with directing the subsequent adaptive immunity [15]

  • In vitro studies showed that ethanol extracts of A. gigas roots suppressed the production of pro-inflammatory mediators in monocytes and macrophages [13]

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Summary

Introduction

The innate immune system orchestrates an immediate early response to the invading microbe. Macrophages are involved in curtailing inflammation and repairing damaged tissues, especially in the resolution phase [3]. These macrophages express anti-inflammatory cytokines (IL-10), immunomodulatory enzymes (arginase-1), growth factors (VEGF-A), and matrix metalloproteinases [4]. In this context, the spatiotemporal balance among the functional states of macrophages should be tightly regulated to maintain tissue homeostasis; otherwise, it leads to inflammatory diseases, including arthritis, colitis, and sepsis

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