The IRG1-itaconate axis protects from cholesterol-induced inflammation and atherosclerosis.
Yannick CyrFazli K BozalJosé Gabriel Barcia DuránAlexandra A C NewmanLetizia AmadoriPanagiotis SmyrnisMorgane GourvestDayasagar DasMichael GildeaRavneet KaurTracy ZhangKristin M WangRichard Von ItterP Martin SchlegelSamantha D DupuisBernard F SanchezAnn Marie SchmidtEdward A FisherCoen van SolingenChiara GiannarelliKatherine MoorePublished in: Proceedings of the National Academy of Sciences of the United States of America (2024)
Atherosclerosis is fueled by a failure to resolve lipid-driven inflammation within the vasculature that drives plaque formation. Therapeutic approaches to reverse atherosclerotic inflammation are needed to address the rising global burden of cardiovascular disease (CVD). Recently, metabolites have gained attention for their immunomodulatory properties, including itaconate, which is generated from the tricarboxylic acid-intermediate cis-aconitate by the enzyme Immune Responsive Gene 1 (IRG1/ACOD1). Here, we tested the therapeutic potential of the IRG1-itaconate axis for human atherosclerosis. Using single-cell RNA sequencing (scRNA-seq), we found that IRG1 is up-regulated in human coronary atherosclerotic lesions compared to patient-matched healthy vasculature, and in mouse models of atherosclerosis, where it is primarily expressed by plaque monocytes, macrophages, and neutrophils. Global or hematopoietic Irg1 -deficiency in mice increases atherosclerosis burden, plaque macrophage and lipid content, and expression of the proatherosclerotic cytokine interleukin (IL)-1β. Mechanistically, absence of Irg1 increased macrophage lipid accumulation, and accelerated inflammation via increased neutrophil extracellular trap (NET) formation and NET-priming of the NLRP3-inflammasome in macrophages, resulting in increased IL-1β release. Conversely, supplementation of the Irg1 -itaconate axis using 4-octyl itaconate (4-OI) beneficially remodeled advanced plaques and reduced lesional IL-1β levels in mice. To investigate the effects of 4-OI in humans, we leveraged an ex vivo systems-immunology approach for CVD drug discovery. Using CyTOF and scRNA-seq of peripheral blood mononuclear cells treated with plasma from CVD patients, we showed that 4-OI attenuates proinflammatory phospho-signaling and mediates anti-inflammatory rewiring of macrophage populations. Our data highlight the relevance of pursuing IRG1-itaconate axis supplementation as a therapeutic approach for atherosclerosis in humans.
Keyphrases
- cardiovascular disease
- single cell
- oxidative stress
- coronary artery disease
- rna seq
- nlrp inflammasome
- endothelial cells
- drug discovery
- adipose tissue
- genome wide
- end stage renal disease
- newly diagnosed
- ejection fraction
- mouse model
- anti inflammatory
- diabetic rats
- coronary artery
- cardiovascular events
- fatty acid
- cardiovascular risk factors
- case report
- high glucose
- immune response
- dna methylation
- heart failure
- risk factors
- chronic kidney disease
- prognostic factors
- ms ms
- skeletal muscle
- gene expression
- machine learning
- transcription factor
- aortic stenosis
- peritoneal dialysis
- aortic valve
- insulin resistance
- left ventricular
- long non coding rna