Regulated Accumulation of Desmosterol Integrates Macrophage Lipid Metabolism and Inflammatory Responses | Zendy

Nathanael J. Spann | Zendy; Lana X. Garmire | Zendy; Jeffrey G. McDonald | Zendy; David S. Myers | Zendy; Stephen Milne | Zendy; Norihito Shibata | Zendy; Donna Reichart | Zendy; Jesse N. Fox | Zendy; Iftach Shaked | Zendy; Daniel Heudobler | Zendy; Christian R.H. Raetz | Zendy; Elaine W. Wang | Zendy; Samuel Kelly | Zendy; M. Cameron Sullards | Zendy; Robert Cushman Murphy | Zendy; Alfred H. Merrill | Zendy; Heather A. Brown | Zendy; Edward A. Dennis | Zendy; Andrew C. Li | Zendy; Klaus Ley | Zendy; Sotirios Tsimikas | Zendy; Eoin Fahy | Zendy; Shankar Subramaniam | Zendy; Oswald Quehenberger | Zendy; David W. Russell | Zendy; Christopher K. Glass | Zendy

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Regulated Accumulation of Desmosterol Integrates Macrophage Lipid Metabolism and Inflammatory Responses

Author(s) -

Nathanael J. Spann,

Lana X. Garmire,

Jeffrey G. McDonald,

David S. Myers,

Stephen Milne,

Norihito Shibata,

Donna Reichart,

Jesse N. Fox,

Iftach Shaked,

Daniel Heudobler,

Christian R.H. Raetz,

Elaine W. Wang,

Samuel Kelly,

M. Cameron Sullards,

Robert Cushman Murphy,

Alfred H. Merrill,

Heather A. Brown,

Edward A. Dennis,

Andrew C. Li,

Klaus Ley,

Sotirios Tsimikas,

Eoin Fahy,

Shankar Subramaniam,

Oswald Quehenberger,

David W. Russell,

Christopher K. Glass

Publication year - 2012

Publication title -

cell

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 26.304

H-Index - 776

eISSN - 1097-4172

pISSN - 0092-8674

DOI - 10.1016/j.cell.2012.06.054

Subject(s) - biology , foam cell , macrophage , inflammation , lipid metabolism , proinflammatory cytokine , desmosterol , transcriptome , microbiology and biotechnology , liver x receptor , homeostasis , reprogramming , cell , cholesterol , gene expression , immunology , biochemistry , gene , transcription factor , sterol , nuclear receptor , in vitro

Inflammation and macrophage foam cells are characteristic features of atherosclerotic lesions, but the mechanisms linking cholesterol accumulation to inflammation and LXR-dependent response pathways are poorly understood. To investigate this relationship, we utilized lipidomic and transcriptomic methods to evaluate the effect of diet and LDL receptor genotype on macrophage foam cell formation within the peritoneal cavities of mice. Foam cell formation was associated with significant changes in hundreds of lipid species and unexpected suppression, rather than activation, of inflammatory gene expression. We provide evidence that regulated accumulation of desmosterol underlies many of the homeostatic responses, including activation of LXR target genes, inhibition of SREBP target genes, selective reprogramming of fatty acid metabolism, and suppression of inflammatory-response genes, observed in macrophage foam cells. These observations suggest that macrophage activation in atherosclerotic lesions results from extrinsic, proinflammatory signals generated within the artery wall that suppress homeostatic and anti-inflammatory functions of desmosterol.

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