Mechanisms of foam cell formation in atherosclerosis

Chistiakov, Dimitry A.; Melnichenko, Alexandra А.; Myasoedova, Veronika A.; Grechko, Andrey V.; Orekhov, Alexander N.

doi:10.1007/s00109-017-1575-8

Cited by 463 publications

(378 citation statements)

References 153 publications

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“…Once adherent to the vascular surface, monocytes enter the intima and differentiate into macrophages that take up modified LDL to form foam cells. 34 A recent study elegantly demonstrated that senescent foam cells with reduced telomere length are vital for plaque buildup, and in later stages, plaque remodeling and rupture. 35 These senescent cells show heightened profiles of proatherogenic and proteolytic factors, including IL-1α, TNFα, MMP-3, MMP12, MMP13, MCP-1, and VCAM-1.…”

Section: Atheroscleros Ismentioning

confidence: 99%

Aging‐ and vascular‐related pathologies

Wen

Wong

2018

Microcirculation

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Our aging population is set to grow considerably in the coming decades. In fact, the number of individuals older than 65 years will double by 2050. This projected increase in people living with extended life expectancy represents an inevitable upsurge in the presentation of age-related pathologies. However, our current understanding of the impact of aging on a number of biological processes is unfortunately inadequate. Cardiovascular, cerebrovascular, and neurodegenerative diseases are particularly prevalent in the elderly population. Intriguingly, these pathologies are all associated with vascular dysfunction, suggesting that the process of aging can induce structural and functional impairments in vascular networks. Together with elevated cell senescence, pre-existing comorbidities, and the emerging concept of age-associated inflammatory imbalance, impaired vascular functions can significantly increase one's risk in acquiring age-related diseases. In this short review, we highlight some current clinical and experimental evidence of how biological aging contributes to three vascular-associated pathologies: atherosclerosis, stroke, and Alzheimer's disease.

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Section: Atheroscleros Ismentioning

confidence: 99%

Aging‐ and vascular‐related pathologies

Wen

Wong

2018

Microcirculation

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“…Atherosclerosis and its complications rank as the leading cause of cardiovascular mortality with the hallmarks of lipid deposition and inflammatory response. The oxidative modification of sequestered lipoproteins triggers the migration of circulating monocytes into the subendothelial space and differentiation into macrophages, which rapidly engulf modified LDL and transform into foam-cell formation (1)(2)(3). Macrophages that accumulate in atherosclerotic plaques seem to have a diminished capacity to migrate.…”

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confidence: 99%

CTRP13 inhibits atherosclerosis via autophagy‐lysosome‐dependent degradation of CD36

Wang

Liang

et al. 2018

FASEB j.

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C1q/tumor necrosis factor-related protein 13 (CTRP13) is a secreted adipokine that can ameliorate abnormal glucose and lipid metabolism. However, the functional role of CTRP13 in the development of atherosclerotic plaques has yet to be described. In this study, we collected blood samples from patients of coronary artery diseases and apolipoprotein E (ApoE) mice that were fed a Western diet for 12 wk to induce atherosclerosis and found that serum CTRP13 level was decreased. En face staining of aortas and aortic sinus in ApoE mice showed that ectopic CTRP13 infusion in vivo dramatically decreased lesion areas, as well as reduced inflammatory responses with less macrophage content. In primary peritoneal macrophages in vitro, CTRP13 supplement reduced oxidized LDL uptake, foam-cell formation, and trapping, together with the suppressed cluster of differentiation 36 (CD36) protein levels. Reduced CD36 protein level was attributed to the autophagy-lysosome-dependent degradation of CD36 at the post-transcriptional level. The blocking of autophagy-lysosome induction could increase CD36 protein level, foam-cell formation, and migration, thus abolishing the protective effects of CTRP13 on atherosclerosis. In summary, these findings define CTRP13 as a novel approach for preventing atherosclerotic plaque formation via modulation of lipid uptake and foam-cell migration.-Wang, C., Xu, W., Liang, M., Huang, D., Huang, K. CTRP13 inhibits atherosclerosis via autophagy-lysosome-dependent degradation of CD36.

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“…VSMCs are a source of foam cells, which are the defining pathologic characteristic of atherosclerotic plaques (22). Intracellular lipid homeostasis reflects a balance of cholesterol uptake, endogenous synthesis, and cholesterol export.…”

Section: Discussionmentioning

confidence: 99%

SCAPknockdown in vascular smooth muscle cells alleviates atherosclerosis plaque formationviaup‐regulating autophagy inApoE^−/−mice

Chen

Tan

et al. 2018

FASEB j.

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Sterol regulatory element binding protein (SREBP) cleavage‐activating protein (SCAP) is a cholesterol sensor that plays a critical role in regulating intracellular cholesterol levels, but the association between SCAP and foam cell formation in vascular smooth muscle cells (VSMCs) is poorly understood. Using tissue‐specific SCAP knockdown in apolipoprotein E (ApoE)−/− mice, we sought to search the mechanism through which SCAP signaling affects VSMC foam cell development. VSMC‐specific SCAP knockdown mice were generated by Cre/LoxP‐mediated gene targeting in ApoE−/− mice. Breeding sCAPflox/flox mice with SM22α‐Cre mice resulted in no viable offspring with the homozygote SM22‐Cre: SCAPflox/flox genotype due to embryonic lethality. We found that the heterozygote SM22α‐Cre:SCAPflox/+: ApoE−/− mice fed a Western diet for 12 wk had significantly fewer atherosclerotic plaques in their aortas than the control mice due to reduced cholesterol uptake and synthesis. Furthermore, we found that autophagy in VSMCs was increased in SM22α‐Cre:SCAPflox/+:ApoE−/− mice. Similarly, in vitro, SCAP knockdown in human coronary artery VSMCs by RNA interference reduced lipid accumulation and increased autophagy under LDL cholesterol loading. SCAP knockdown in VSMCs reduced oxidative stress and increased AMPK phosphorylation, which contributed to the up‐regulation of autophagy in vivo and in vitro. VSMC‐specific SCAP knockdown decreased the lipid accumulation and intracellular oxidative stress, increased excessive lipid clearance by enhancing lipid autophagy mediated by the reactive oxygen species/AMPK pathway in VSMCs, and consequently alleviated atherosclerosis plaque formation.—Li, D., Chen, A., Lan, T., Zou, Y., Zhao, L., Yang, P., Qu, H., Wei, L., Varghese, Z., Moorhead, J. F., Chen, Y., Ruan, X. Z. SCAP knockdown in vascular smooth muscle cells alleviates atherosclerosis plaque formation via up‐regulating autophagy in ApoE−/− mice. FASEB J. 33, 3437–3450 (2019). http://www.fasebj.org

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Mechanisms of foam cell formation in atherosclerosis

Cited by 463 publications

References 153 publications

Aging‐ and vascular‐related pathologies

Aging‐ and vascular‐related pathologies

CTRP13 inhibits atherosclerosis via autophagy‐lysosome‐dependent degradation of CD36

SCAPknockdown in vascular smooth muscle cells alleviates atherosclerosis plaque formationviaup‐regulating autophagy inApoE^−/−mice

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Mechanisms of foam cell formation in atherosclerosis

Cited by 463 publications

References 153 publications

Aging‐ and vascular‐related pathologies

Aging‐ and vascular‐related pathologies

CTRP13 inhibits atherosclerosis via autophagy‐lysosome‐dependent degradation of CD36

SCAPknockdown in vascular smooth muscle cells alleviates atherosclerosis plaque formationviaup‐regulating autophagy inApoE−/−mice

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SCAPknockdown in vascular smooth muscle cells alleviates atherosclerosis plaque formationviaup‐regulating autophagy inApoE^−/−mice