Monocyte and Macrophage Lipid Accumulation Results in Down-Regulated Type-I Interferon Responses

Lisa Willemsen; Hung-Jen Chen; Cindy P A A van Roomen; Guillermo R Griffith; Ricky Siebeler; Annette E Neele; Jeffrey Kroon; Marten A Hoeksema; Menno P J de Winther

doi:10.3389/fcvm.2022.829877

Monocyte and Macrophage Lipid Accumulation Results in Down-Regulated Type-I Interferon Responses

Front Cardiovasc Med. 2022 Feb 10:9:829877. doi: 10.3389/fcvm.2022.829877. eCollection 2022.

Authors

Lisa Willemsen¹, Hung-Jen Chen¹, Cindy P A A van Roomen¹, Guillermo R Griffith¹, Ricky Siebeler¹, Annette E Neele¹, Jeffrey Kroon², Marten A Hoeksema¹, Menno P J de Winther¹

Affiliations

¹ Department of Medical Biochemistry, Experimental Vascular Biology, Amsterdam Cardiovascular Sciences, Amsterdam Infection and Immunity, University of Amsterdam, Amsterdam, Netherlands.
² Department of Experimental Vascular Medicine, Amsterdam Cardiovascular Sciences, University of Amsterdam, Amsterdam, Netherlands.

Abstract

Macrophages are critical components of atherosclerotic lesions and their pro- and anti-inflammatory responses influence atherogenesis. Type-I interferons (IFNs) are cytokines that play an essential role in antiviral responses and inflammatory activation and have been shown to promote atherosclerosis. Although the impact of type-I IFNs on macrophage foam cell formation is well-documented, the effect of lipid accumulation in monocytes and macrophages on type-I IFN responses remains unknown. Here we examined IFN stimulated (ISG) and non-ISG inflammatory gene expression in mouse and human macrophages that were loaded with acetylated LDL (acLDL), as a model for foam cell formation. We found that acLDL loading in mouse and human macrophages specifically suppressed expression of ISGs and IFN-β secretion, but not other pro-inflammatory genes. The down regulation of ISGs could be rescued by exogenous IFN-β supplementation. Activation of the cholesterol-sensing nuclear liver X receptor (LXR) recapitulated the cholesterol-initiated type-I IFN suppression. Additional analyses of murine in vitro and in vivo generated foam cells confirmed the suppressed IFN signaling pathways and suggest that this phenotype is mediated via down regulation of interferon regulatory factor binding at gene promoters. Finally, RNA-seq analysis of monocytes of familial hypercholesterolemia (FH) patients also showed type-I IFN suppression which was restored by lipid-lowering therapy and not present in monocytes of healthy donors. Taken together, we define type-I IFN suppression as an athero-protective characteristic of foamy macrophages. These data provide new insights into the mechanisms that control inflammatory responses in hyperlipidaemic settings and can support future therapeutic approaches focusing on reprogramming of macrophages to reduce atherosclerotic plaque progression and improve stability.

Keywords: atherosclerosis; cholesterol; foam cell formation; immunometabolism; inflammation; interferon response; macrophage; monocyte.