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Review
. 2023 Oct 1;34(5):189-195.
doi: 10.1097/MOL.0000000000000888. Epub 2023 Aug 9.

Macrophage inflammarafts in atherosclerosis

Shenglin Li  1 Juliana M Navia-PelaezSoo-Ho ChoiYury I Miller
Affiliations
Review

Macrophage inflammarafts in atherosclerosis

Shenglin Li et al. Curr Opin Lipidol. .

Abstract

Purpose of review: Advances in single cell techniques revealed a remarkable diversity in macrophage gene expression profiles in atherosclerosis. However, the diversity of functional processes at the macrophage plasma membrane remains less studied. This review summarizes recent advances in characterization of lipid rafts, where inflammatory receptors assemble, in macrophages that undergo reprogramming in atherosclerotic lesions and in vitro under conditions relevant to the development of atherosclerosis.

Recent findings: The term inflammarafts refers to enlarged lipid rafts with increased cholesterol content, hosting components of inflammatory receptor complexes assembled in close proximity, including TLR4-TLR4, TLR2-TLR1 and TLR2-CD36 dimers. Macrophages decorated with inflammarafts maintain chronic inflammatory gene expression and are primed to an augmented response to additional inflammatory stimuli. In mouse atherosclerotic lesions, inflammarafts are expressed primarily in nonfoamy macrophages and less in lipid-laden foam cells. This agrees with the reported suppression of inflammatory programs in foam cells. In contrast, nonfoamy macrophages expressing inflammarafts are the major inflammatory population in atherosclerotic lesions. Discussed are emerging reports that help understand formation and persistence of inflammarafts and the potential of inflammarafts as a novel therapeutic target.

Summary: Chronic maintenance of inflammarafts in nonfoamy macrophages serves as an effector mechanism of inflammatory macrophage reprogramming in atherosclerosis.

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References

    1. Miller YI, Navia-Pelaez JM, Corr M, Yaksh TL. Lipid rafts in glial cells: role in neuroinflammation and pain processing. J Lipid Res 2020; 61:655–666.
    1. Navia-Pelaez JM, Agatisa-Boyle C, Choi SH, et al. Differential expression of inflammarafts in macrophage foam cells and in nonfoamy macrophages in atherosclerotic lesions. Arterioscler Thromb Vasc Biol 2023; 43:323–329.
    1. Tabas I, Bornfeldt KE. Macrophage phenotype and function in different stages of atherosclerosis. Circ Res 2016; 118:653–667.
    1. Zernecke A, Erhard F, Weinberger T, et al. Integrated single-cell analysis based classification of vascular mononuclear phagocytes in mouse and human atherosclerosis. Cardiovasc Res 2023; 119:1676–1689.
    1. Pan H, Xue C, Auerbach BJ, et al. Single-cell genomics reveals a novel cell state during smooth muscle cell phenotypic switching and potential therapeutic targets for atherosclerosis in mouse and human. Circulation 2020; 142:2060–2075.

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