Desmosterol suppresses macrophage inflammasome activation and protects against vascular inflammation and atherosclerosis.
Xinbo ZhangJeffrey G McDonaldBinod AryalAlberto Canfrán-DuqueEmily L GoldbergElisa AraldiWen DingYuhua FanBonne M ThompsonAbhishek K SinghQian LiGeorge TellidesJose Ordovás-MontanesRolando García MilianVishwa Deep DixitElina IkonenYajaira SuárezCarlos Fernández-HernandoPublished in: Proceedings of the National Academy of Sciences of the United States of America (2021)
Cholesterol biosynthetic intermediates, such as lanosterol and desmosterol, are emergent immune regulators of macrophages in response to inflammatory stimuli or lipid overloading, respectively. However, the participation of these sterols in regulating macrophage functions in the physiological context of atherosclerosis, an inflammatory disease driven by the accumulation of cholesterol-laden macrophages in the artery wall, has remained elusive. Here, we report that desmosterol, the most abundant cholesterol biosynthetic intermediate in human coronary artery lesions, plays an essential role during atherogenesis, serving as a key molecule integrating cholesterol homeostasis and immune responses in macrophages. Depletion of desmosterol in myeloid cells by overexpression of 3β-hydroxysterol Δ 24 -reductase (DHCR24), the enzyme that catalyzes conversion of desmosterol to cholesterol, promotes the progression of atherosclerosis. Single-cell transcriptomics in isolated CD45 + CD11b + cells from atherosclerotic plaques demonstrate that depletion of desmosterol increases interferon responses and attenuates the expression of antiinflammatory macrophage markers. Lipidomic and transcriptomic analysis of in vivo macrophage foam cells demonstrate that desmosterol is a major endogenous liver X receptor (LXR) ligand involved in LXR/retinoid X receptor (RXR) activation and thus macrophage foam cell formation. Decreased desmosterol accumulation in mitochondria promotes macrophage mitochondrial reactive oxygen species production and NLR family pyrin domain containing 3 (NLRP3)-dependent inflammasome activation. Deficiency of NLRP3 or apoptosis-associated speck-like protein containing a CARD (ASC) rescues the increased inflammasome activity and atherogenesis observed in desmosterol-depleted macrophages. Altogether, these findings underscore the critical function of desmosterol in the atherosclerotic plaque to dampen inflammation by integrating with macrophage cholesterol metabolism and inflammatory activation and protecting from disease progression.
Keyphrases
- oxidative stress
- single cell
- adipose tissue
- low density lipoprotein
- induced apoptosis
- cell cycle arrest
- coronary artery
- cardiovascular disease
- reactive oxygen species
- immune response
- rna seq
- cell death
- dendritic cells
- signaling pathway
- endoplasmic reticulum stress
- physical activity
- type diabetes
- poor prognosis
- coronary artery disease
- high throughput
- cell proliferation
- pulmonary artery
- binding protein
- fatty acid
- inflammatory response
- replacement therapy